Movatterモバイル変換

[0]ホーム
URL:

US8187625B2 - Cross-linked gelatin composition comprising a wetting agent - Google Patents

Cross-linked gelatin composition comprising a wetting agentDownload PDF

Info

Publication number
US8187625B2
US8187625B2US10/068,812US6881202AUS8187625B2US 8187625 B2US8187625 B2US 8187625B2US 6881202 AUS6881202 AUS 6881202AUS 8187625 B2US8187625 B2US 8187625B2
Authority
US
United States
Prior art keywords
cross
wetting agent
gelatin
hemostatic
biocompatible
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Fee Related, expires
Application number
US10/068,812
Other versions
US20030028140A1 (en
Inventor
Richard J. Greff
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Boston Scientific Scimed Inc
Original Assignee
Scimed Life Systems Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Scimed Life Systems IncfiledCriticalScimed Life Systems Inc
Priority to US10/068,812priorityCriticalpatent/US8187625B2/en
Assigned to SUB-Q, INC.reassignmentSUB-Q, INC.ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: GREFF, RICHARD J.
Publication of US20030028140A1publicationCriticalpatent/US20030028140A1/en
Assigned to PACIFIC VENTURE GROUP II, L.P., CRAGG, ANDREW H., WALLACE, GEORGE, FEUCHTER, BRUCE, BOSTON SCIENTIFIC CORPORATION, ALLEN FAMILY TRUST DATED 10/12/81, PEQUOT PRIVATE EQUITY FUND II, L.P., HARTZLER, GEOFFREY O., PVG ASSOCIATES II, L.P., KINGSBURY CAPITAL PARTNERS, L.P. IV, KINGSBURY CAPITAL PARTNERS, L.P. IIIreassignmentPACIFIC VENTURE GROUP II, L.P.NOTE AND WARRANT PURCHASE AGREEMENTAssignors: SUB-Q, INC.
Assigned to BOSTON SCIENTIFIC SCIMED, INC.reassignmentBOSTON SCIENTIFIC SCIMED, INC.ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS).Assignors: SUB-Q, INC.
Priority to US13/477,541prioritypatent/US8524270B2/en
Application grantedgrantedCritical
Publication of US8187625B2publicationCriticalpatent/US8187625B2/en
Priority to US13/967,472prioritypatent/US8821918B2/en
Adjusted expirationlegal-statusCritical
Expired - Fee Relatedlegal-statusCriticalCurrent

Links

Images

Classifications

Definitions

Landscapes

Abstract

Disclosed is a biocompatible, hemostatic, cross-linked gelatin composition comprising a biocompatible material comprising cross-linked gelatin and a sufficient amount of wetting agent to permit uniform wetting of the sponge in the presence of an aqueous solution.

Description

CROSS REFERENCE TO RELATED APPLICATIONS
This application claims priority to U.S. Provisional Patent Application Ser. No. 60/275,420, filed on Mar. 12, 2001, which application is incorporated by reference herein in its entirety.
BACKGROUND OF INVENTIONField of the Invention
This invention is directed to a biocompatible, hemostatic cross-linked gelatin composition comprising cross-linked gelatin and a sufficient amount of wetting agent to permit uniform wetting of the gelatin in the presence of an aqueous solution. This invention is further directed towards methods of decreasing the hydration time of cross-linked gelatin by incorporating a biocompatible wetting agent into the gelatin. This invention further relates to a kit of parts for preparing a biocompatible, hemostatic cross-linked gelatin composition comprising a sterile syringe and non-hydrated, biocompatible, pledget comprising a cross-linked gelatin and a wetting agent.
References
The following patent applications and patents are cited and/or referenced in this application as superscript numbers:
  • 1 Correll, et al., Proc. Soc. Exp. Biol. N.Y., 58:233 (1945).
  • 2 Correll, et al., Surg. Gyn. and Obst., 82:585 (1945).
  • 3 Correll, et al., U.S. Pat. No. 2,465,357, Therapeutic Sponge and Method of Making, issued Mar. 29, 1949.
  • 4 Correll, et al., U.S. Pat. No. 2,507,244, Surgical Gelatin Dusting Powder and Process for Preparing Same, issued May 9, 1950.
  • 5 Studer, et al., U.S. Pat. No. 2,558,395, Undenatured Gelatin Hemostatic Sponge Containing Thrombin, issued Jun. 26, 1951.
  • 6 Sieger, et al., U.S. Pat. No. 2,899,362, Hemostatic Sponges and Method of Preparing Same, issued Aug. 11, 1959.
  • 7 Song, et al., U.S. Pat. No. 5,399,361, Collagen-containing Sponges as Drug Delivery Compositions for Proteins, issued Mar. 21 1995.
  • 8 Cragg, et al., U.S. Pat. No. 6,071,301, Device and Method for Facilitating Hemostasis of a Biopsy Tract, issued Jun. 6, 2000.
  • 9 Cragg, et al., U.S. Pat. No. 6,086,607, Device and Method for Facilitating Hemostasis of a Biopsy Tract, issued Jul. 11, 2000.
  • 10 Cragg, et al., U.S. Pat. No. 6,162,192, System and Method for Facilitating Hemostasis of Blood Vessel Punctures with Absorbable Sponge, issued Dec. 19, 2000.
  • 11 Pawelchak, et al., U.S. Pat. No. 4,292,972, Lyophilized Hydrocolloid Foam, issued Oct. 6, 1981.
  • 12 Sawyer, U.S. Pat. No. 4,238,480, Method for Preparing an Improved Hemostatic Agent and Method of Employing the Same, issued Dec. 9, 1980.
  • 13 Sawyer, U.S. Pat. No. 4,404,970, Hemostatic Article and Method for Preparing and Employing the Same, issued Sep. 20, 1983.
All of the above references are herein incorporated by reference in their entirety to the same extent as if each individual reference was specifically and individually indicated to be incorporated by reference in its entirety.
State of the Art
Cross-linked gelatin, often in the form of gelatin foam, gelatin film or gelatin sponges, has been used as a hemostatic agent since its development by Correll in 1945.1-4Such hemostatic sponges or foams are used routinely to pack wounds, absorb blood and stop bleeding. They are often left in place to be bioabsorbed over a period of weeks to months. In addition, medicaments, such as antibiotics, growth factors and thrombus enhancing agents, have been incorporated into the cross-linked gelatin to enhance the in vivo properties of the composition.5-7
To use, the hemostatic sponge is placed onto or into the wound, whereupon it absorbs blood or other fluids, expands to pack and compress the wound, and initiates a rapid clotting response. However, to achieve complete fluid absorption, rapid expansion, effective wound compression, and vigorous clotting action, the sponge must first be pre-hydrated or wetted, usually with sterile saline, before placement in the wound. This pre-hydration step, often accompanied with gentle compression and/or massaging of the sponge, can be time consuming and troublesome, often yielding non-uniform results at a critical moment in patient care. (See, for example, Directions for Use provided with Gelfoam®—available from Pharmacia Upjohn).
The hydrated sponge can then be compressed by hand and inserted or tamped into the wound. One particular wound suitable for use by hydrated sponges is a puncture site such as a puncture wound resulting from catheter insertion or a biopsy needle. When so used, the art describes ejection of a pledget of cross-linked gelatin from a syringe into the puncture site.8-10
Critical to the ejection process is the flowability of the pledget from the syringe assembly and retention of its structural integrity during insertion into the body. Specifically, ejection of the pledget from the syringe assembly is preferably conducted with, at most, moderate pressure to ensure accurate placement in vivo. Efficient ejection of the pledget, in turn, relates to the flowability of the cross-linked gelatin through the syringe assembly. Higher fluid content pledgets are believed to correlate with enhanced flowability and, accordingly, it is desirable to maintain as high a fluid absorbability content in the sterilized pledget as possible.
Likewise, it is critical that the structural integrity of the pledget is substantially maintained as it is ejected from the syringe assembly when placed in vivo in order to ensure that portions of the pledget are not torn or otherwise separated from the pledget. This criticality is particularly important when the pledget is placed over a blood vessel puncture in order to avoid unintended thrombosis of the vessel. Structural integrity of the gelatin composition of the pledget under pressure is believed to correlate with the tensile strength of the composition and, accordingly, it is desirable to maintain as high a tensile strength in the sterilized pledget as possible.
In addition, it is desirable to perform hydration of the pledgets in the sterile environment of an injection syringe or syringe assembly by addition of a sterile saline solution to the syringe. Such a hydration process is complicated by the potential of distortions in the pledget due to a lack of uniformity and consistency in the rate of hydration of the pledget. Such distortions could cause unanticipated difficulties in fitting the pledget into the identified wound, e.g., puncture. In addition, the length of time normally needed to hydrate the pledget would typically prohibit such a hydration process. Accordingly, it is desired to obtain a quicker, more uniform hydration of the pledget to ensure predictability of the size and shape of the pledget and to facilitate hydration of the pledget inside the injection syringe.
SUMMARY OF THE INVENTIONAmendment to Brief Description of the Drawings
FIG. 1. is a side view of a hemostatic compound delivery system.
This invention is directed to a biocompatible, hemostatic, cross-linked gelatin composition which has a wetting agent incorporated therein. In particular, this invention is directed to a biocompatible material comprising a cross-linked gelatin and a sufficient amount of wetting agent to permit uniform wetting of the gelatin in the presence of an aqueous solution. This invention further relates to methods of using this composition to decrease the hydration time of a hemostatic, cross-linked gelatin composition. This invention further relates to a kit of parts for preparing a biocompatible, hemostatic, cross-linked gelatin composition comprising a sterile syringe and non-hydrated, biocompatible, pledget comprising a cross-linked gelatin and a wetting agent.
Applicants have surprisingly and unexpectedly found that wetting agents can be incorporated into a cross-linked gelatin composition, improving their use as, e.g., a hemostatic sponge.
Applicants have further surprisingly found that the incorporation of wetting agents into a hemostatic, cross-linked gelatin composition decreases the hydration time needed to prepare the gelatin for use. Incorporation of the wetting agent into the cross-linked gelatin composition provides for one or more of improved fluid absorption, gelatin expansion and wound compression.
Applicants have also surprisingly found that hemostatic, cross-linked gelatin compositions with wetting agents incorporated therein are more uniformly lubricated when ejected as a pledget from a syringe assembly and less likely to suffer damage to the structural integrity of the pledget. Such pledgets are also more quickly hydrated, allowing for hydration of the pledget inside the injection syringe. Further, the pledgets made according to the invention are more uniformly hydrated, and less likely to become distorted during the hydration process.
Accordingly, in one embodiment, this invention is directed to a biocompatible, hemostatic, cross-linked gelatin composition comprising a cross-linked gelatin and a sufficient amount of wetting agent to permit uniform wetting of the gelatin in the presence of an aqueous solution.
In one embodiment, the incorporation of the wetting agent into the cross-linked gelatin can be achieved by mixing or impregnating the gelatin with wetting agent prior to foaming. In this embodiment, the wetting agent can comprise from about 0.01 to 10 weight percent of the gelatin and preferably from about 0.1 to 10 weight percent.
In another embodiment, the incorporation of the wetting agent into the cross-linked gelatin can be achieved by coating the wetting agent over the surface of a gelatin sponge. In this embodiment, a solution of wetting agent and liquid solvent carrier is prepared wherein the wetting agent comprises from about 0.01 to 20 percent of the solution and preferably from about 1 to 10 weight percent. The solution is coated over the surface of the sponge, then the liquid solvent carrier is evaporated. After evaporation, the wetting agent comprises from about 0.01 to about 5 weight percent of the gelatin sponge and preferably from about 0.1 to about 5 weight percent.
In both embodiments, the biocompatible, hemostatic sponge can be bioabsorbable. The sponge can also include one or more compositions selected from the group consisting of growth factors, thrombus enhancing agents, and antimicrobial agents.
In one of its method aspects, the invention is directed to a method for decreasing the hydration time of a cross-linked gelatin composition which method comprises, prior to hydration of said cross-linked gelatin, incorporating a biocompatible wetting agent with said cross-linked gelatin.
The biocompatible, hemostatic sponge of the present invention can be sterilized and packaged to facilitate use in surgical procedures.
Accordingly, in another of its aspects, this invention is directed to a kit of parts for preparing a biocompatible, hemostatic, cross-linked gelatin composition comprising a syringe or syringe assembly and a non-hydrated pledget, said pledget comprising a cross-linked gelatin and wetting agent.
DETAILED DESCRIPTION OF THE INVENTION
This invention is directed to a biocompatible, hemostatic, cross-linked gelatin composition which has a wetting agent incorporated therein. In particular, this invention is directed to a biocompatible material comprising a cross-linked gelatin and a sufficient amount of wetting agent incorporated therein to permit uniform wetting of the sponge in the presence of an aqueous solution and to methods of using this composition to decrease the hydration time of the gelatin composition. Prior to describing this invention in further detail, the following terms will first be defined.
Definitions
As used herein, the following terms have the following meanings:
The term “cross-linked gelatin” refers to well known gelatin foams or sponges which are cross-linked with a conventional cross-linking agent such as formaldehyde as described in the art by Correll.1-3The term “cross-linked gelatin composition” refers to compositions comprising cross-linked gelatin. Such compositions often include other components such as a medicament8-10or a second polymer such as collagen13and starch6.
The term “growth factors” refers to those medicaments which are conventionally employed to facilitate tissue growth such as the endothelial wall of a punctured blood vessel or biopsy tract. Examples of suitable growth factors include PDGF, EGF, FGF, IGF's 1 and 2, TGF and the like.
The term “thrombus enhancing agents” refers to those medicaments which are conventionally employed to facilitate thrombus formation at a puncture site such as at the endothelial wall of a punctured blood vessel or a biopsy tract. Examples of suitable thrombus enhancing agents include thrombin, fibrinogen, Factor XIII and other coagulation factors.
The term “antimicrobial agent” refers to agents which destroy microbes (i.e., bacteria, fungi, viruses and microbial spores) thereby preventing their development and pathogenic action. Preferred antimicrobial agents include antibiotics and antiviral agents and, in particular, antibiotics. Other preferred antimicrobials include, for example, iodine containing materials such as PVP-I2, chlorhexidene, and the like.
The term “packaging element” refers to those packaging components used to encase the cross-linked gelatin and include, by way of example, boxes, syringes, envelopes, tubings, catheters, introducers and the like. The packaging elements may comprise glass, plastic, ceramics, cardboard, paper products and the like.
The term “wetting agent” refers to a biocompatible agent which facilitates or enhances the hydration or lubrication of a hemostatic sponge. Examples of suitable wetting agents include polyoxyalkylenes (such as BASF Pluronics™, UCC Carbowaxes™, PEGs™), ether capped polyoxyalkylenes, e.g., polyoxyethylene lauryl ether, ester capped polyoxyalkylenes, e.g., polyoxyethylene stearate, sorbitan esters (such as certain products called Span™ and Tween™), phosphatides (such as lecithin), alkyl amines, glycerin, water soluble polymers such as polyethylene oxides, carboxymethyl cellulose, polyvinyl alcohol, and polyvinyl pyrrolidone, surfactants such as alky (C6-C20) sulfate salts, e.g. sodium lauryl sulfate, aryl (C6-C10) sulfate salts, and alkaryl (C7-C24) sulfate salts, and the like.
Compositions
The compositions of this invention include biocompatible hemostatic, cross-linked gelatin compositions comprising a cross-linked gelatin composition and a sufficient amount of wetting agent to permit uniform wetting of the gelatin in the presence of an aqueous solution.
The wetting agent is utilized in an amount sufficient to enhance the hydration and/or lubrication of the composition. When the wetting agent is incorporated into the cross-linked gelatin, the wetting agent will comprise from about 0.01 to about 10 weight percent based on the total weight of the composition and preferably from about 0.1 to 10 weight percent. When the wetting agent is coated onto the surface of the cross-linked gelatin, the wetting agent will comprise from about 0.01 to about 20 weight percent, based on the total weight of the applied solution (preferably from about 1 to 20 weight percent), and 0.01 to 5 weight percent based on the total weight of the gelatin composition after evaporation of the liquid solvent of the applied solution (and preferably from about 0.1 to 5 weight percent).
In a preferred embodiment, the cross-linked gelatin composition further comprises a medicament such as an antimicrobial agent (e.g., an antibiotic), growth factors, thrombus enhancing agents, and the like or a property modifying agent such as a wetting agent. Mixtures of medicaments and property modifying agents can also be used. Suitable medicaments can be mixed with or impregnated into the cross-linked gelatin composition prior to sterilization procedures.
When employed, the medicament is utilized in an amount sufficient for its intended purpose, e.g., an antimicrobially effective amount, an amount sufficient to induce thrombus formation, and an amount sufficient to promote growth. The specific amount employed relates to the effectiveness of the medicament, the disease condition of the patient being treated, the age and weight of the patient, the location of the disease and other factors well within the purview of the attending clinician.
Prior to administration of the biocompatible, hemostatic, cross-linked gelatin to the patient, the gelatin will be sterilized. Sterilization can be achieved by, for example, heat or E-beam sterilization. Biocompatible wetting agents will typically be incorporated into or coated onto the cross-linked gelatin composition prior to the sterilization procedure. E-beam sterilization of a cross-linked gelatin composition is described in U.S. Provisional Patent Application Ser. No. 60/275,391, filed Mar. 12, 2001, entitled “Methods for Sterilizing Cross-Linked Gelatin Compositions”, which application is incorporated herein by reference in its entirety. Heat sterilization of a cross-linked gelatin composition is described in U.S. Pat. No. 2,465,357.3
In the embodiment described inFIG. 1, a pledget of the cross-linked gelatin composition of the present invention can be inserted into asyringe assembly10 comprising a holdingchamber14, an injection port which comprises aluer hub20, and anejection port22 which is attached to acannula24. The syringe assembly containing thepledget16 can packaged and sterilized. Then,sterile saline12 can be added to the holdingchamber14 in a sufficient amount to hydrate thepledget16. Once the pledget is hydrated, thepledget16 can be transferred into thecannula24 attached to theejection port22.
The incorporation of wetting agents into the cross-linked gelatin composition can allow for rapid, uniform wetting of the gelatin and elimination of the pre-hydration process. The wetting agent can be added and dissolved (or dispersed) directly into the hemostat chemical formulation, preferably just before the foaming process. An amount of wetting agent ranging from about 0.01 to 10 percent based on the weight of the gelatin material, and preferably from 0.1 to 10 percent, can be used. Processes for manufacturing a hemostatic sponge are disclosed in U.S. Pat. No. 2,465,3573and U.S. Pat. No. 2,507,2444.
Alternatively, the wetting agent could be dissolved (or dispersed) in a non-aqueous liquid solvent (e.g., ethanol, isopropanol, acetone and the like) coated onto the cross-linked gelatin composition and the liquid solvent removed by evaporation. In another embodiment, the wetting agent and liquid solvent mixture could be applied onto the gelatin composition and the foam compressed. The liquid solvent would then be removed by evaporation. When the wetting agent is coated over the gelatin composition, the concentration of the wetting agent in the liquid solvent is preferably from about 0.01 to 20 percent and preferably from 1 to 20 weight percent and more preferably 1 to 10 weight percent.
Suitable biocompatible wetting agents are commercially available and include, for example, sodium lauryl sulfate, Pluronic™ F-68, Pluronic™ F-38, Pluronic™ P-105, Pluronic™-10R5,Tween™ 20, Tween™ 60, Tween™ 85, Brij™ 35, Brij™ 78, Myrj™ 52, PEG™ 600, glycerin and the like.
In addition, biocompatible wetting agents can be incorporated into biocompatible collagen hemostatic sponges (e.g., Actifoam™) to improve their wetting times in the manner and concentrations set forth above. Suitable wetting agents include Tween™ 20 (1% in isopropanol) and Pluronic™ P-105 (1% in isopropanol).
EXAMPLES
The following examples are set forth to illustrate the claimed invention and are not to be construed as a limitation thereof.
In these examples, unless otherwise indicated, all temperatures are in degrees Centrigrade and all percents are weight percents based on the total weight of the composition. Similarly, the following abbreviations are employed herein and are as defined below. Unless defined, the abbreviations employed have their generally accepted meaning:
cc=cubic centimeter
cm=centimeter
EtOH=ethanol
g=gram
IPA=isopropyl alcohol
min.=minute
mm=millimeter
mL=milliliters
pcs=pieces
RH=relative humidity
RO water=reversed osmosis water
RPM=rotations per minute
sec=seconds
wt=weight
Example 1Comparison of Hydration Time of Cross-linked Gelatin with Wetting Agent Incorporated Therein vs. Cross-linked Gelatin Without Wetting Agent
The purpose of this example is to demonstrate the feasibility of different agents in reducing the hydration time of a cross-linked gelatin having a variety of candidate wetting agents incorporated into the gelatin prior to foaming (Gelatin Composition 1A). In this example, the surfactant was added to the solution used to prepare the cross-linked gelatin foam.
The results of the amount of time required to wet the gelatin was compared to the hydration time of a cross-linked gelatin which does not have any candidate wetting agents incorporated therein (Comparative Gelatin Composition 1B).
A. Preparation of Gelatin Composition 1A
Gelatin Composition 1A was prepared as follows. A stock solution of 5% pigskin gelatin in purified bottled water was prepared by heating to 60° C. with constant stirring. The solution was cooled to 37° C. and 0.01% formalin added. This was incubated for two hours. To produce a 10% surfactant to gelatin ratio (i.e., 10% loading), 1.5 grams of surfactant was dissolved in 20 grams of water, and this solution added to 280 gram aliquots of the stock gelatin solution.
Foam was produced by whipping air into the warm mixture for about 2 minutes using a kitchen blender. The whipping ceased when the foam peaked. The gelatin foam was then transferred to screens and contained within metal shells until firm, about 10-15 minutes. The foam was dried at 32.2° C. (90° F.) and 18% RH, which took about 24-36 hours. Test samples were prepared by cutting the skin from the dried foam buns and cutting cubes of about 1.5-2.0 cm from central locations in the bun. For additional information regarding the preparation of such gelatin compositions, see U.S. Pat. Nos. 2,465,357 and 2,507,244.
The following candidate wetting agents were each incorporated into the gelatin prior to foaming:
1. Polyacrylamide (weight average molecular weight of about 1500) (as a sample of a cationic wetting agent)
2. Sodium lauryl sulfate (as a sample of a anionic wetting agent)
3. Pluronic™ F-68 (poly(ethylene oxide)-co-(propylene oxide) block), (as a sample of a non-ionic wetting agent—number average molecular weight of about 8400) (commercially available from BASF Corp.)
4. Tween™ 20 (polyoxyethylene sorbitan monolaurate), (as a sample of a non-ionic wetting agent—molecular weight of approximately 1227)
5. PEG™ (600) (poly(ethylene glycol), (as a sample of a non-ionic wetting agent—molecular weight of about 600)
6. Glycerin (as a sample of a non-ionic wetting agent)
B. Preparation of Comparative Gelatin Composition 1B
Comparative Gelatin Composition 1B was prepared as above except for omission of the wetting agent.
C. Comparison of the Foam Properties and Hydration Time of Cross-linked Gelatin with Wetting Agent Incorporated Therein vs. Gelatin Without Wetting Agent
(1) Foam Properties
Most of the gelatin compositions produced a smooth, white, meringue-like foam, which dried into a high, rigid, compressible bun.
Gelatin compositions 1A produced with lauryl sulfate, Pluronic™ F-68,Tween™ 20 and 30% lauryl sulfate candidate wetting agents were softer and less compressible. These compositions also displayed some loss of foam height and an increase in cell size and voids. TheTween™ 20 and 30% lauryl sulfate formulations demonstrated the most collapse and increase in cell size and voids.
(2) Hydration
Table 1 sets forth the hydration times for the Gelatin Compositions 1A and the Comparative Gelatin Compositions. Hydration was tested in both uncompressed and compressed (comp.) foams. The concentration of candidate wetting agent in each composition is indicated as a percent loading. Specifically, the percent loading refers to the weight percent of the wetting agent based on gelatin in the composition before foaming based on a 300 mL solution containing 5% gelatin.
The Gelatin Compositions 1A with the lauryl sulfate (30% loading),Tween™ 20 and Pluronic™ F-68 wetting agents yielded a startling reduction in hydration time and about 3-10 seconds (versus 6 minutes for the Comparative Gelatin Composition 1B (control)). The amount of water absorbed was somewhat reduced for the 30% lauryl sulfate containing sample. It was basically unchanged for the other two compositions.
Unless otherwise noted, all samples were the aggregate of 3 pieces.
TABLE 1
Hydration Times for Gelatin
Compositions 1A and Comparative Gelatin Compositions
Hydration
TimeDryWetWet/Dry
Wetting Agent(min)Weight (g)Weight (g)(3 pcs)
Comparative Gelatin6.5-7.00.133.7429
Composition 1B
(0% loading)
Comparative Gelatin6.0-6.50.124.2335
Composition 1B
(0% loading)
(Comp 15—2 mm)
Gelatin Composition 1A>200.14NDND
Polyacrylamide Wetting
Agent (10% loading)
Gelatin Composition 1A>200.16NDND
Polyacrylamide Wetting
Agent (10% loading)
(Comp 15—2mm)
Gelatin Composition 1A45 sec0.244.3018
Lauryl sulfate Wetting
Agent (10% loading)
Gelatin Composition 1A45 sec0.447.5517
Lauryl sulfate Wetting
Agent (10% loading)
(Comp 20—2 mm)
Gelatin Composition 1A10-15 sec0.183.0117 (1 pc)
Lauryl sulfate Wetting
Agent (30% loading)
Gelatin Composition 1A10 sec0.173.0418 (1 pc)
Lauryl sulfate Wetting
Agent (30% loading)
(Comp 15—1 mm)
Gelatin Composition 1A3-5 sec0.174.1324
Pluronic F-68 Wetting
Agent (10% loading)
Gelatin Composition 1A3-5 sec0.153.7325
Pluronic F-68 Wetting
Agent (10% loading)
(Comp 15—3 mm)
Gelatin Composition 1A5 sec0.3710.90 29
Tween 20 Wetting Agent
(10% loading)
Gelatin Composition 1A5 sec0.288.0829
Tween 20 Wetting Agent
(10% loading)
(Comp 10—2 mm)
Gelatin Composition 1A4.50.185.1529
PEG 600 Wetting Agent
(10% loading)
Gelatin Composition 1A3.50.226.0127
PEG 600 Wetting Agent
(10% loading)
(Comp 20—2 mm)
Gelatin Composition 1A4.50.255.1321
Glycerin Wetting Agent
(10% loading)
Gelatin Composition 1A3.50.256.7127
Glycerin Wetting Agent
(10% loading)
(Comp 20—2 mm)
Comparative Gelatin5.50.164.7230
Composition 1B
(0% loading)
The wet/dry ratio reported is the wet weight over the dry weight which provides a ratio of the amount of water absorbed per unit weight of dry material.
The above data indicates that all of the candidates used, with the exception of polyacrylamide, act as wetting agents per this invention. On the other hand, the increase in wetting time provided by using polyacrylamide indicates that this material is not a suitable wetting agent.
The above data of the different agents used, little or no change in the wet/dry ratio occurred with the use of eitherTween™ 20 or PEG™ 600; modest lowering of the wet/dry ratio occurred with the use of Pluronic™ F-68 and Glycerin; and somewhat greater lowering of the wet/dry ratio occurred with the use of lauryl sulfate.
Example 2Comparison of Hydration Times Cross-linked Gelatin Compositions with Wetting Agent Coating vs. Cross-linked Gelatin Compositions without a Wetting Agent Coating
The purpose of this example is to demonstrate the reduction in hydration time of a cross-linked gelatin composition containing different non-ionic wetting agents (Gelatin Composition 2A) and forming a surfactant coating on the preformed cross-linked gelatin foam composition. Specifically, in this example, the wetting agents were coated onto the cross-linked gelatin composition in the following manner: the wetting agent was added to a solvent, the cross-linked gelatin composition was added to the resulting solution, the soak time used was 10 seconds or 1 minute, as indicated below, the cross-linked gelatin composition was removed, excess liquid drained, and then the solvent was allowed to evaporate.
The hydration time required to wet these compositions was compared to the hydration time of a cross-linked gelatin composition without such a wetting agent coating (Comparative Gelatin Composition 2B (no coating) and Comparative Gelatin Composition 2C (carrier solvent coating)).
A. Preparation of Gelatin Composition 2A
Gelatin Composition 2A was prepared as follows. First, Comparative Gelatin Composition 1B, as set forth in Example 1, was prepared.
Second, ten percent solutions of each of the following wetting agents were prepared in isopropanol (2-Propanol, ACS reagent (Aldrich Cat. #19076-4)) in 30 cc screw cap vials.
1.Tween ™ 20 (polyoxyethylene (20) sorbitan monolaurate)
(Aldrich Cat. #27434-8)
2.Tween ™ 60 (polyoxyethylene (20) sorbitan monostearate)
(Aldrich Cat. #37425-3)
3.Tween ™ 85 (polyoxyethylene (20) sorbitan trioleate) (Aldrich
Cat. #38890-4)
4.Brij ™ 35 (polyoxyethylene (23) lauryl ether) (Aldrich Cat.
#85836-6) (Sigma)
5.Myrj ™ 52 (polyoxyethylene (40) stearate) (Aldrich Cat.
#P3440) (BASE)
6.Brij ™ 78 (polyoxyethylene (23) steryl ether) (Sigma
#23600-4)
A 2×2×0.6 cm piece of Gelatin Composition 2A was placed into each vial and the vial inverted to soak the composition with the solution. This was repeated for each solution. Two contact/soak times were employed, 10 seconds and one minute.
The coated Gelatin Compositions 2A were then removed, drained of excess liquid and air dried overnight.
B. Preparation of Comparative Gelatin Composition 2B and 2C
Comparative Gelatin Composition 2B (untreated) was prepared as set forth for Comparative Gelatin Composition 1B in Example 1.
Comparative Gelatin Composition 2C (carrier solvent coating) was prepared as follows. A 2×2×0.6 cm piece of Comparative Gelatin Composition 1B (as set forth in Example 1) was placed into a 30 cc screw cap vial of isopropanol and the vial inverted to soak the composition with the solution. Two contact/soak times were employed, 10 seconds and one minute. After soaking, the gelatin compositions were then air dried overnight.
C. Comparison of Hydration Times
Dry samples of each of the Gelatin Compositions 2A and the Comparative Gelatin Compositions 2B and 2C were compressed to about 0.1 cm and dropped into a 250 mL beaker containing 100 mL of RO water.
The time for each gelatin composition to reach full hydration was measured with a digital stopwatch. Hydrated samples were weighed and reweighed to assure full hydration. Hydration was also determined by monitoring when the composition turned from opaque to translucent.
The results of this evaluation are shown in Table 2. Where two values are given, duplicate runs were made.
TABLE 2
Hydration Times for Gelatin Composition
2A and Comparative Gelatin Compositions 2B and 2C
Soak Time in
Wetting AgentHydration
Gelatin CompositionSolutionTimeWet/Dry Wt.
Comparative Gelatin06, 6 min28, 33
Composition 2B
Gelatin Composition 2A10sec20, 25 sec49, 35
Tween 20 Wetting Agent
Gelatin Composition 2A1.0min15, 20 sec49, 58
Tween 20 Wetting Agent
Gelatin Composition 2A10 sec3, 1.5 min41, 44
Tween 60 Wetting Agent
Gelatin Composition 2A1.0min24, 35 sec38, 31
Tween 60 Wetting Agent
Gelatin Composition 2A10 sec30, 30 sec41, 45
Tween 85 Wetting Agent
Gelatin Composition 2A1.0 min35, 35 sec46, 34
Tween 85 Wetting Agent
Gelatin Composition 2A10sec15, 20 sec38, 26
Myrj 52 Wetting Agent
Gelatin Composition 2A1.0 min40, 40 sec37, 29
Myrj 52 Wetting Agent
Gelatin Composition 2A10 sec15, 15 sec55, 42
Brij 35 Wetting Agent
Gelatin Composition 2A1.0 min40, 40 sec52, 33
Brij 35 Wetting Agent
Gelatin Composition 2A10 sec15, 15 sec38, 39
Brij 78 Wetting Agent
Gelatin Composition 2A1.0min20, 20 sec43, 42
Brij 78 WettingAgent
Comparative Gelatin
10 sec3 min40
Composition 2C
Comparative Gelatin1.0 min3 min40
Composition 2C
The wet/dry ratio reported is the wet weight over the dry weight which provides a ratio of the amount of water absorbed per unit weight of dry material.
All samples of cross-lined gelatin, treated or not, yielded very large and similar uptakes for water (wet/dry weight). Also, as evident above, the best wetting agents were deemed those that produced the most rapid hydration, e.g.,Tween™ 20, Brij™ 35 and Brij™ 78.
Example 3Demonstration of Improved Hydration Time for Cross-linked Gelatins with Wetting Agent Coatings Containing Ethanol and Isopropanol Carrier Solvents
The purpose of this example is to demonstrate that the improved hydration time achieved for cross-linked gelatins coated with non-aqueous wetting agents as per Example 2 above were independent of the solvent used to coat the gelatin.
Specifically, gelatin composition 3A was prepared in the same manner as gelatin composition 2A. The wetting agent coating solution comprises a selected wetting agent and a carrier solvent of either ethanol or isopropanol. Soak contact time of the foam in the wetting solution was about 10 seconds each.
After the coating layer has dried, the gelatin compositions were compressed and soaked in a 250 mL beaker containing 100 mL of RO water. The hydration times were measured as in Example 2.
1.Tween ™ 20 (polyoxyethylene (20) sorbitan monolaurate)
(Aldrich Cat. #27434-8)
2.Pluronic ™ F-68 (poly(ethylene oxide)-co-(propylene oxide)
block), (as a sample of a non-ionic wetting agent-- average
molecular weight of about 8400) (commercially available from
BASF Corp.)
3.Pluronic ™ P-105 (poly(ethylene oxide)-co-(propylene oxide)
polymer), (as a sample of a non-ionic wetting agent-- average
molecular weight of about 6500) (commercially available from
BASF Corp.)
4.Pluronic-10R5 ™ (poly(ethylene oxide)-co-(propylene oxide)
polymer), (as a sample of a non-ionic wetting agent-- average
molecular weight of about 4550) (commercially available from
BASE Corp.).
5.Pluronic-F38 ™ (poly(ethylene oxide)-co-(propylene oxide)
block), (as a sample of a non-ionic wetting agent-- average
molecular weight of about 5000) (commercially available from
BASE Corp.).
Hydration times for the compositions are set forth in Table 3 below. Where multiple values are given, multiple runs were made.
TABLE 3
Hydration Times for Gelatin Compositions 3A
Wetting Agent
Used in GelatinCarrier
Composition 3ASolventHydration Times
Tween
203% ETOH10, 15; 10, 15, 15sec
Tween
203% IPA20, 20; 10, 10, 15sec
Tween
2010% ETOH10, 10sec
Tween
2010% IPA10, 10 sec
F-383% ETOH40, 40, 40 sec
F-383% IPA30, 45, 45 sec
F-683% ETOH30, 45, 45 sec
F-683% IPA20, 25, 20 sec
P-1053% ETOH10, 15, 10 sec
P-1053% IPA10, 10, 10 sec
10R53% ETOH10, 20, 20 sec
10R53% IPA10, 10, 10 sec
The average wet/dry ratio for the above samples was approximately 44 with a range of from 39-56 wherein this ratio is calculated by the wet weight over the dry weight which provides a ratio of the amount of water absorbed per unit weight of dry material.
The above data demonstrates that there is no appreciable difference in the hydration time of the coated cross-linked gelatin using different solvents to coat the gelatin.
However, the solvent employed should be non-aqueous to the extent that water irreversible damages the foam. Preferably, the non-aqueous solvent is ethanol and/or isopropanol since methanol causes some degradation of the foam properties and acetone exhibits a disagreeable odor.
Example 4Hydration Times for Cross-linked Gelatin Compositions with Wetting Agent Coating of Varying Concentrations
This example examines the effect of wetting agent concentration on hydration time used to coat the cross-linked gelatin composition.
Specifically, cross-linked gelatin compositions with wetting agent coatings were prepared as in Example 2. The wetting agent coating solutions were prepared with concentrations of the selected wetting agents of 0.1, 1.0, 3.0 and 10.0%. The hydration times were measured on compressed samples, in the manner set forth in Example 2.
All of the wetting agents and concentrations demonstrated rapid hydration times, although at the highest concentration of 10%, the hydration time was somewhat reduced. The results are set forth in Table 4 below. Where multiple values are given, multiple runs were made.
TABLE 4
Hydration Times for Cross-Linked Gelatin
Compositions with Wetting Agent Coatings of Varying Concentrations
Wetting
Agent UsedHydration Times at Wetting Agent Concentration
in Coating0.10%1.00%3.00%10.00%
Tween ™
2015, 10; 60,15, 10; 15,20, 10sec20, 10 sec
25, 15sec10, 10; 10
sec
Brij ™ 3510, 10, 10;15, 10, 10;10, 20, 1520, 30, 30
35, 20, 2030, 20 secsecsec
sec
Brij ™ 7810, 15, 1010, 10; 2510, 10 sec
secsec
P-10515, 15sec10, 10; 1010, 10 sec
sec
10R515, 15sec10, 10sec10, 10 sec
The wet/dry ratio reported is the wet weight over the dry weight which provides a ratio of the amount of water absorbed per unit weight of dry material.
The above data demonstrates that the concentration of wetting agent employed in the coating solution does not materially affect the hydration time of the coated cross-linked gelatin.
Example 5Hydration Times for Cross-linked Gelatin Compositions with Wetting Agent of Varying Concentrations Incorporated Therein
This example evaluates the effect of wetting agent concentration used during the formation of a gelatin foam composition on both the hydration time and the wet/dry ratio. This example differs from the previous example in that the wetting agent is added to the composition prior to foam formation as per Example 1 rather than coating a prior formed cross-linked gelatin foam with the wetting agent as per Examples 2-4.
Specifically, cross-linked gelatin compositions with wetting agents incorporated therein were prepared as in Example 1 except that 0.02 weight percent of formalin was used and wherein the wetting agent was added to the gelatin composition prior to foam formation. The wetting agent coating solutions were prepared with concentrations set forth in Table 5.
The hydration times for these gelatin compositions were measured by manually compressing each cut sample and dropping it into a beaker containing 150 mL of tap water. Hydration was complete when the foam turned translucent and were measured on compressed samples, in the manner set forth in Example 2. Hydration time of a control, similar to Comparative Gelatin Example 2B, was also measured.
The hydration times are set forth in the Table 5 below.
TABLE 5
Wt.
WettingConcentra-HydrationWet/
AgenttionFoam WetFoam DryTimeDry
Tween ™
20  5%¾in.in.2-3secNA
Tween ™
20  3%½in.in.2-3sec23.4
Tween ™ 20  1%¾in.¼in.2-3sec24.0
Tween ™ 200.10%¾in.in.5sec41.5
Tween ™ 60  3%no foamNANA
Tween ™ 85  3%no foamNANA
Myrj ™ 52  3%no foamNANA
Brij ™ 35  3%in.¼in.2-3sec16.5
Brij ™ 78  3%½in.in.2-3sec12.0
F-68  3%1in.¼in.2-3sec19.7
Control  0%in.in. 8mm45.8
These results indicate that gelatin foam compositions with wetting agents did not achieve the same level of foam formation as compared to the control. Upon drying, foam heights for these compositions were further reduced, with the lowest concentration of surfactant causing less height reduction.
The compositions with the wetting agents incorporated therein also tended to be softer and more resilient, more fibrous and with larger irregular cells than the control compositions. Again, the lowest concentration of surfactant (0.1%) gave foams closer to the control.
All gelatin foams with wetting agent incorporated therein demonstrated very rapid and complete hydration. Hydration was complete within 2-3 seconds for the surfactant gelatin samples compared to about 8 minutes for the control. At the 0.1% level, the presence of the surfactant was sufficient to dramatically improve hydration times.
Unfortunately, water uptake was significantly diminished for all surfactant samples, except those with the lowest concentration of surfactant. Mechanical strength of all the samples (wet or dry) was excellent, and equal to that of the control.
Based on the above data, when the wetting agent is incorporated prior to cross-linked gelatin foam formation, very low concentrations of wetting agent are preferred. Moreover, the data indicates minimal impact of low concentrations of wetting agent on reduced hydration time indicating that such low concentrations advantageously provide for a composition closer to control in many properties but surprisingly have excellent hydration times as compared to control.
Preferred wetting agents as demonstrated in this example utilizing the addition of wetting agent prior to foam formation should not prevent foam sponge formation of the cross-linked gelatin.
Example 6
This example demonstrates that the incorporation of a wetting agent into a gelatin composition does not deleteriously effect the clotting ability of the gelatin composition as compared to control. A partial thromboplastin test (PTT) was employed. The PTT assay is a general screening assay for the detection of coagulation abnormalities in the intrinsic coagulation pathway. This is particularly important because, notwithstanding improved hydration time, a cross-linked gelatin composition having an adverse effect on blood clotting would be contra-indicated for use, e.g., as a hemostatic sponge.
Specifically, in this example, fresh whole human blood was drawn at AppTec Laboratory Services using vacutainer tubes containing sodium citrate. The citrated whole blood was spun down. The plasma was separated from the red blood cells, pooled into a polypropylene test tube, and stored on ice. This plasma was used as the exposure medium for testing.
The comparison sample, test tube, reference material and controls were placed in polypropylene tubes and exposed to plasma (determined by the 1 mL/4 cm2exposure ratio) for 15 minutes at 37±1° C. in an agitating water bath at 60 RPM. The volume of 0.3 mL of plasma was used to saturate the test and comparison articles prior to exposure. At the end of the incubation period, the plasma was removed from the materials. The plasma samples were placed on ice and tested on the Cascade M4.
The results are set forth in Tables 6 and 7 below.
TABLE 6
Exposure RatiosCoagulation Time (seconds)
Surface% of Neg
ArticleArea (cm2)(mL)Assay ValuesAve.Control
Cross-linked4.01.0300/226.7/300275.6 92
Gelatin - Ex.
2B
Gelfoam4.01.0300/300/300300100
(Pharmacia-
Upjohn)
Positive4.01.0NA39.9 13
Control,
Black Rubber
Reference4.01.0NA174.3 58
Material, Latex
Tubing
NegativeNA1.0NA300NA
Control,
Human
Plasma
TABLE 7
Exposure RatiosCoagulation Time (seconds)
Surface% of Neg
ArticleArea (cm2)(ml)Assay ValuesAve.Control
Cross-linked4.01.0300/208.2/300269.4 90
Gelatin - Ex
2A
(0.3% Tween
20)
Gelfoam4.01.0300/300/300300100
(Pharmacia-
Upjohn)
Positive4.01.0NA39.9 13
Control,
Black Rubber
Reference4.01.0NA174.3 58
Material, Latex
Tubing
NegativeNA1.0NA300NA
Control,
Human
Plasma
If coagulation does not occur within 300 seconds, the result is reported as “300 sec.”).
The above data demonstrates that the compositions of this invention exhibit substantially equivalent effects on clotting time as compared to control and, accordingly, it was concluded that these compositions are compatible for use as, e.g., hemostatic sponges.
Example 7
This example evaluates the histopathologic results of a total of 2 arterial femoral puncture sites from one pig, using the compositions of this invention. The objective of this evaluation was to assess the acute and chronic outcome of femoral puncture sites following closure with the compositions of this invention delivered into the tissue tract adjacent to the vessel puncture using a cannula delivery tube. The puncture wound in the right femoral artery was sealed with cross-linked gelatin composition comprising 0.1% Tween 20 obtained from solvent coating of the composition per Example 2 above. The puncture wound in the left femoral artery was sealed with cross-linked gelatin composition comprising 0.3% Tween 20 obtained from solvent coating of the composition per Example 2 above. Subsequently, approximately 2-4 weeks later, the animal was sacrificed, the arteries adjacent the femoral puncture site were excised and fixed in formalin.
Specifically, the formalin-fixed arterial explants were trimmed in the area of interest every 3 mm into 11 to 14 segments (sections 1 to 14). The sections' sequence was started at the proximal end of each explant. The sections were embedded in paraffin, sectioned at approximately 5 microns three times serially, and stained with Hematoxylin and Eosin (HE), Masson's Trichrome (MT), and Verhoeff's Van Gieson (VVG) stain, respectively. Histologic evaluation was performed and data were recorded.
A 1 to 5 grading scale was utilized, where 1 is minimal, 2 is mild, 3 is moderate, 4 is marked, and 5 is severe. Loss of endothelium was graded according to circumferential spread of the change. The change of endothelium loss spanned approximately up to 20% of the circumference in grade 1, 20-40% in grade 2, 40-60% in grade 3, 60-80% in grade 4 and more than 80% in grade 5. Necrosis of the media was graded according to depth extension. The change of media necrosis extended into approximately up to 20% of the media thickness in grade 1, 20-40% in grade 2, 40-60% in grade 3, 60-80% in grade 4 and more than 80% in grade 5.
1-Animal 3094G—Right Femoral Artery
Gross Observations: The segment of artery was 52 mm long. There were no significant gross changes in the intact explant. Trimming revealed sub-occlusive thrombosis in most sections (1 through 8) and partial thrombosis insections 9 and 10. The delivery tract could not be seen grossly.
Microscopic Observations: The puncture site was observed in sections 9 and 10 (24 and 27 mm from origin). There was transmural laceration with regeneration and fibrosis of the edges. From these lacerated sites and the corresponding intimal areas of more proximal sections a partially organized thrombus projected into the lumen and was nearly occluding the lumen. There was mineralization of the media in a sub-intimal position (sections 1, 2, 7, 8, 9), due to localized media pressure necrosis (dystrophic mineralization). Mineralization was also observed in the organizing thrombus. There was slight to mild partial loss of endothelium in the proximal sections (sections 1-7) that was considered to be the result of erosion associated with termination catheterization. In approximately the proximal ⅔ of the explant (sections 1-10) there was fibrosis of the media, most likely due to pressure necrosis at the time of treatment. The implant was not observed. There was mature connective tissue in the adventitia possibly corresponding to the treatment tract. These microscopic observations are consistent with arterial needle puncture and healing.
2-Animal 3094G—Left Femoral Artery
Gross Observations: The segment of artery was 50 mm long. There were no significant gross changes in the intact explant.
Microscopic Observations: Transmural laceration (puncture site) was observed in section 8 (18-21 mm, recut 3) and was characterized by bifocal laceration across the vessel with proliferation of fibrous granulation tissue across the lumen dividing the pre-existing arterial wall into two symmetrically placed remnants. The residual lumen was confined to one of the arterial remnants. The lumen was constructed (moderate stensosis) by intimal fibrous proliferation at the puncture site. There was mineralization of the external elastic lamina adjacent to the laceration site. There was moderate fibrosis in the adventitia at the laceration site and in a separate area in the more distant adventitial tissue that most likely corresponds to the puncture tract. There was no residual implant material and there was no significant inflammatory response in the tract. There was minimal to mild loss of endothelium that was considered to be the result of erosion associated with termination catheterization.
The access tract produced by the catheter was found in the vascular wall in both samples as a localized fibrosis in the adventitia and focal transmural fibrosis. The left artery displayed bifocal transmural laceration and healing by fibrous connective tissue and media regeneration bridging across the lumen, indicating focal puncture through opposite sides of the vessel. There was no significant occlusive thrombosis in the left artery but focal moderate stenosis associated with intimal hyperplasia at the puncture site was present. The right artery there was sub-occlusive thrombosis that proceeded from the puncture site and extended proximally. There was evidence of pronounced architectural disruption and media necrosis due to mechanical trauma to the vessel wall at the puncture site, believed to be responsible for thrombosis. No residual foam test material was observed. These microscopic observations are consistent with arterial needle puncture and healing.
The above data demonstrates that the compositions of this invention are well tolerated in vivo.
Example 8
This example evaluates the cytotoxicity of the compositions of this invention as compared to prior art compositions, i.e., in the absence of a wetting agent. In this example, samples were tested in the ISO agarose overlay cytotoxicity test—a test well known in the art for determining cytotoxicity potential. Specifically, samples were placed onto petri dishes, in triplicate, containing agarose the surface of which contains a monolayer of L-929 mouse fibroblast cells which are sensitive to cytotoxic agents. Subsequently, the samples were evaluated for reactivity and grade depending upon the amount of cellular damage or death directly beneath and/or surrounding the material. The scoring is based on the following:
0=no zone under or around sample
1=some malformed or degenerated cells under sample
2=zone limited to area under sample
3=zone extends 0.5 to 1.0 cm beyond sample
4=zone extends greater than 1.0 cm
In this example, a score of 0-2 is deemed to be non-toxic; a score of 3 is deemed to be weakly or moderately toxic; and a score of 4 is strongly toxic.
The results of this evaluation are summarized below in Table 8:
TABLE 8
SampleScore
Cross-linked gelatin w/o surfactant0
Cross-linked gelatin with Tween 20
(prepared by Example 2—isopropanol)
0.3% Tween 200
1.0% Tween 201,1 (two triplicate runs)
Cross-linked gelatin with Pluronic P-105
(prepared by Example 2 isopropanol)
0.3% Pluronic P-1050,0 (two triplicate runs)
1.0% Pluronic P-1050,0 (two triplicate runs)
The above results demonstrate that the compositions of this invention, as tested in this example, are non-cytotoxic.
From the foregoing description, various modifications and changes in the above described methods will occur to those skilled in the art. All such modifications coming within the scope of the appended claims are intended to be included therein.

Claims (13)

US10/068,8122001-03-122002-02-04Cross-linked gelatin composition comprising a wetting agentExpired - Fee RelatedUS8187625B2 (en)

Priority Applications (3)

Application NumberPriority DateFiling DateTitle
US10/068,812US8187625B2 (en)2001-03-122002-02-04Cross-linked gelatin composition comprising a wetting agent
US13/477,541US8524270B2 (en)2001-03-122012-05-22Cross-linked gelatin composition coated with a wetting agent
US13/967,472US8821918B2 (en)2001-03-122013-08-15Cross-linked gelatin composition comprising a wetting agent

Applications Claiming Priority (2)

Application NumberPriority DateFiling DateTitle
US27542001P2001-03-122001-03-12
US10/068,812US8187625B2 (en)2001-03-122002-02-04Cross-linked gelatin composition comprising a wetting agent

Related Child Applications (1)

Application NumberTitlePriority DateFiling Date
US13/477,541ContinuationUS8524270B2 (en)2001-03-122012-05-22Cross-linked gelatin composition coated with a wetting agent

Publications (2)

Publication NumberPublication Date
US20030028140A1 US20030028140A1 (en)2003-02-06
US8187625B2true US8187625B2 (en)2012-05-29

Family

ID=23052214

Family Applications (3)

Application NumberTitlePriority DateFiling Date
US10/068,812Expired - Fee RelatedUS8187625B2 (en)2001-03-122002-02-04Cross-linked gelatin composition comprising a wetting agent
US13/477,541Expired - Fee RelatedUS8524270B2 (en)2001-03-122012-05-22Cross-linked gelatin composition coated with a wetting agent
US13/967,472Expired - Fee RelatedUS8821918B2 (en)2001-03-122013-08-15Cross-linked gelatin composition comprising a wetting agent

Family Applications After (2)

Application NumberTitlePriority DateFiling Date
US13/477,541Expired - Fee RelatedUS8524270B2 (en)2001-03-122012-05-22Cross-linked gelatin composition coated with a wetting agent
US13/967,472Expired - Fee RelatedUS8821918B2 (en)2001-03-122013-08-15Cross-linked gelatin composition comprising a wetting agent

Country Status (3)

CountryLink
US (3)US8187625B2 (en)
EP (1)EP1389125B1 (en)
WO (1)WO2002072128A1 (en)

Cited By (2)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US8821918B2 (en)2001-03-122014-09-02Boston Scientific Scimed Inc.Cross-linked gelatin composition comprising a wetting agent
US11679177B2 (en)2017-08-082023-06-20Baxter International Inc.Polymeric compositions, delivery devices, and methods

Families Citing this family (50)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US6162192A (en)1998-05-012000-12-19Sub Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6183497B1 (en)*1998-05-012001-02-06Sub-Q, Inc.Absorbable sponge with contrasting agent
US6071300A (en)*1995-09-152000-06-06Sub-Q Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US6315753B1 (en)*1998-05-012001-11-13Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US7625352B1 (en)1998-05-012009-12-01Sub-Q, Inc.Depth and puncture control for system for hemostasis of blood vessel
US20010045575A1 (en)*1998-05-012001-11-29Mark AshbyDevice and method for facilitating hemostasis of a biopsy tract
US6984219B2 (en)1999-09-232006-01-10Mark AshbyDepth and puncture control for blood vessel hemostasis system
US7700819B2 (en)2001-02-162010-04-20Kci Licensing, Inc.Biocompatible wound dressing
US7763769B2 (en)2001-02-162010-07-27Kci Licensing, Inc.Biocompatible wound dressing
WO2002087636A1 (en)*2001-03-122002-11-07Sub-Q, Inc.Methods for sterilizing cross-linked gelatin compositions
US7008440B2 (en)*2001-11-082006-03-07Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US6863680B2 (en)*2001-11-082005-03-08Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US7192436B2 (en)2001-11-082007-03-20Sub-Q, Inc.Pledget-handling system and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US7025748B2 (en)*2001-11-082006-04-11Boston Scientific Scimed, Inc.Sheath based blood vessel puncture locator and depth indicator
US7037323B2 (en)*2001-11-082006-05-02Sub-Q, Inc.Pledget-handling system and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US7923431B2 (en)*2001-12-212011-04-12Ferrosan Medical Devices A/SHaemostatic kit, a method of preparing a haemostatic agent and a method of promoting haemostatis
US7455680B1 (en)2002-11-042008-11-25Boston Scientific Scimed, Inc.Apparatus and method for inhibiting blood loss
BR0317237A (en)*2002-12-112005-11-01Ferrosan As Sampling or collecting device, kit, uses of a device and a kit, and methods for decreasing the amount of a marker in a sample area, for qualitatively or quantitatively sampling an area for the content of a marker and for grow microorganisms or mammalian cells collected
US20040122349A1 (en)2002-12-202004-06-24Lafontaine Daniel M.Closure device with textured surface
US8709038B2 (en)2002-12-202014-04-29Boston Scientific Scimed, Inc.Puncture hole sealing device
EP1631262A4 (en)*2003-06-122010-05-05Boston Scient Ltd An Irish Co IMPROVED SYSTEM AND METHOD FOR FACILITATING HEMOSTASE USING AN ABSORBABLE SPONGE
US7942897B2 (en)2003-07-102011-05-17Boston Scientific Scimed, Inc.System for closing an opening in a body cavity
US7927626B2 (en)*2003-08-072011-04-19Ethicon, Inc.Process of making flowable hemostatic compositions and devices containing such compositions
US8440225B2 (en)*2003-08-072013-05-14Ethicon, Inc.Process of making flowable hemostatic compositions and devices containing such compositions
US20060019868A1 (en)2004-01-302006-01-26Pendharkar Sanyog MHemostatic compositions and devices
US7875043B1 (en)2003-12-092011-01-25Sub-Q, Inc.Cinching loop
AR054637A1 (en)*2004-01-302007-07-11Ferrosan As AEROSOLS AND HEMOSTATIC COMPOSITIONS
US7109163B2 (en)*2004-01-302006-09-19Ethicon, Inc.Hemostatic compositions and devices
US8992454B2 (en)*2004-06-092015-03-31Bard Access Systems, Inc.Splitable tip catheter with bioresorbable adhesive
US8119160B2 (en)2004-06-292012-02-21Ethicon, Inc.Hemostatic compositions and devices
RU2369408C2 (en)*2004-07-092009-10-10Ферросан А/СHemostatic composition comprising hyaluronic acid
JP5569398B2 (en)2008-02-292014-08-13フェッローサン メディカル ディバイス エー/エス Device for promoting hemostasis and / or wound healing
EP2252335B1 (en)2008-03-032013-04-24Omrix Biopharmaceuticals Ltd.A gelatin sponge comprising an active ingredient, its preparation and use
JP5562324B2 (en)*2008-04-032014-07-30ザイモジェネティクス, インコーポレイテッド Hemostasis microsphere
DE102008020197A1 (en)*2008-04-152009-10-22Gelita Ag Fast wettable, hydrocolloid-containing material, process for its preparation and its use
SA111320355B1 (en)*2010-04-072015-01-08Baxter Heathcare S AHemostatic sponge
KR102002755B1 (en)2010-06-012019-07-23백스터 인터내셔널 인코포레이티드Process for making dry and stable hemostatic compositions
US9084728B2 (en)2010-06-012015-07-21Baxter International Inc.Process for making dry and stable hemostatic compositions
CN103732265B (en)*2011-08-022016-10-12大日精化工业株式会社Anti medical material and manufacture method thereof
WO2013131520A2 (en)2012-03-062013-09-12Ferrosan Medical Devices A/SPressurized container containing haemostatic paste
CN104349797B (en)2012-06-122017-10-27弗罗桑医疗设备公司Dry hemostatic composition
CA2912357C (en)2013-06-212019-12-31Ferrosan Medical Devices A/SVacuum expanded dry composition and syringe for retaining same
RU2678592C1 (en)2013-12-112019-01-30Ферросан Медикал Дивайсиз А/СDry composition comprising extrusion enhancer
JP6726852B2 (en)2014-10-132020-07-22フェッローサン メディカル ディバイス エー/エス Dry composition for use in hemostasis and wound healing
CA2970710A1 (en)2014-12-242016-06-30Ferrosan Medical Devices A/SSyringe for retaining and mixing first and second substances
EP3316930B1 (en)2015-07-032019-07-31Ferrosan Medical Devices A/SSyringe for mixing two components and for retaining a vacuum in a storage condition
CN105561375B (en)*2016-01-052018-11-30山东省药学科学院A kind of gelatin liquid-absorbent hemostatic sponge and preparation method thereof of dopamine crosslinking
WO2019215274A1 (en)2018-05-092019-11-14Ferrosan Medical Devices A/SMethod for preparing a haemostatic composition
US20250082818A1 (en)*2023-09-082025-03-13Anti-Microbial Savior Bioteq Co., Ltd.Artificial dressing, use of artificial dressing for promoting wound healing and method of manufacturing artificial dressing
CN117065083A (en)*2023-09-282023-11-17上海七木医疗器械有限公司 Absorbable fluid gelatin materials and preparation methods and uses thereof

Citations (180)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US581235A (en)1897-04-20Island
US1578517A (en)1924-12-231926-03-30George N HeinValve piston and barrel construction for hypodermic syringes
US2086580A (en)1935-06-241937-07-13Myron C ShirleyApplicator
US2370319A (en)1944-11-071945-02-27Dohner & LippincottPaper perforator
US2465357A (en)1944-08-141949-03-29Upjohn CoTherapeutic sponge and method of making
US2492458A (en)1944-12-081949-12-27Jr Edgar A BeringFibrin foam
US2507244A (en)1947-04-141950-05-09Upjohn CoSurgical gelatin dusting powder and process for preparing same
US2558395A (en)1947-06-031951-06-26Hoffmann La RocheUndenatured gelatin hemostatic sponge containing thrombin
US2597011A (en)1950-07-281952-05-20Us AgriculturePreparation of starch sponge
US2680442A (en)1952-04-041954-06-08Frank L LinzmayerDisposable suppository casing
US2761446A (en)1955-03-301956-09-04Chemical Specialties Co IncImplanter and cartridge
US2814294A (en)1953-04-171957-11-26Becton Dickinson CoUnit for and method of inhibiting and controlling bleeding tendencies
US2824092A (en)1955-01-041958-02-18Robert E ThompsonProcess of preparation of a gelatincarboxymethyl cellulose complex
US2874776A (en)1954-06-071959-02-24Royal Mcbee CorpPunch and die mechanism
US2899362A (en)1959-08-11Hemostatic sponges and method of
US2997195A (en)1959-07-161961-08-22Yuen Yat ChuenDrinking straws
US3157524A (en)1960-10-251964-11-17Ethicon IncPreparation of collagen sponge
US3358689A (en)1964-06-091967-12-19Roehr Products Company IncIntegral lancet and package
US3411505A (en)1965-12-151968-11-19Paul D. NobisDevice for interrupting arterial flow
US3703174A (en)1970-07-141972-11-21Medidyne CorpMethod and apparatus for catheter injection
US3724465A (en)1971-07-221973-04-03Kimberly Clark CoTampon coated with insertion aid and method for coating
US3736939A (en)1972-01-071973-06-05Kendall & CoBalloon catheter with soluble tip
US4000741A (en)1975-11-031977-01-04The Kendall CompanySyringe assembly
GB1509023A (en)1973-02-121978-04-26Ochsner Med Found AltonSeptal defect closure apparatus
US4098728A (en)1976-01-021978-07-04Solomon RosenblattMedical surgical sponge and method of making same
GB1569660A (en)1976-07-301980-06-18Medline AbOcclusion of body channels
US4211323A (en)1978-12-011980-07-08California Medical Developments, Inc.Disposable diagnostic swab having a stored culture medium
US4218155A (en)1978-02-101980-08-19Etablissements Armor, S.A.Stick for applying a liquid
US4219026A (en)1978-09-151980-08-26The Kendall CompanyBladder hemostatic catheter
US4224945A (en)1978-08-301980-09-30Jonathan CohenInflatable expansible surgical pressure dressing
US4238480A (en)1978-05-191980-12-09Sawyer Philip NicholasMethod for preparing an improved hemostatic agent and method of employing the same
US4292972A (en)1980-07-091981-10-06E. R. Squibb & Sons, Inc.Lyophilized hydrocolloio foam
US4323072A (en)1980-01-181982-04-06Shiley, IncorporatedCannula for a vein distention system
US4340066A (en)1980-02-011982-07-20Sherwood Medical Industries Inc.Medical device for collecting a body sample
US4390018A (en)1980-09-151983-06-28Zukowski Henry JMethod for preventing loss of spinal fluid after spinal tap
US4405314A (en)1982-04-191983-09-20Cook IncorporatedApparatus and method for catheterization permitting use of a smaller gage needle
US4404970A (en)1978-05-191983-09-20Sawyer Philip NicholasHemostatic article and methods for preparing and employing the same
US4515637A (en)1983-11-161985-05-07Seton CompanyCollagen-thrombin compositions
US4573576A (en)1983-10-271986-03-04Krol Thomas CPercutaneous gastrostomy kit
US4587969A (en)1985-01-281986-05-13Rolando GillisSupport assembly for a blood vessel or like organ
US4588395A (en)1978-03-101986-05-13Lemelson Jerome HCatheter and method
US4591094A (en)1983-08-131986-05-27Arthur MorrisFountain
US4619261A (en)1984-08-091986-10-28Frederico GuerrieroHydrostatic pressure device for bleeding control through an inflatable, stitchable and retrievable balloon-net system
US4619913A (en)1984-05-291986-10-28Matrix Pharmaceuticals, Inc.Treatments employing drug-containing matrices for introduction into cellular lesion areas
US4644649A (en)1985-09-261987-02-24Seaman Roy CApparatus for trimming reeds of musical instruments
US4645488A (en)1982-08-121987-02-24Board Of Trustees Of The University Of AlabamaSyringe for extrusion of wetted, particulate material
US4699616A (en)1986-06-131987-10-13Hollister IncorporatedCatheter retention device and method
US4708718A (en)1985-07-021987-11-24Target TherapeuticsHyperthermic treatment of tumors
US4744364A (en)1987-02-171988-05-17Intravascular Surgical Instruments, Inc.Device for sealing percutaneous puncture in a vessel
US4790819A (en)1987-08-241988-12-13American Cyanamid CompanyFibrin clot delivery device and method
US4829994A (en)1987-05-271989-05-16Kurth Paul AFemoral compression device for post-catheterization hemostasis
US4832688A (en)1986-04-091989-05-23Terumo Kabushiki KaishaCatheter for repair of blood vessel
US4836204A (en)1987-07-061989-06-06Landymore Roderick WMethod for effecting closure of a perforation in the septum of the heart
US4839204A (en)1987-05-191989-06-13Yazaki Kakoh Co., Ltd.Resin coated metal pipe having a plane surface for a lightweight structure
US4850960A (en)1987-07-081989-07-25Joseph GrayzelDiagonally tapered, bevelled tip introducing catheter and sheath and method for insertion
US4852568A (en)1987-02-171989-08-01Kensey Nash CorporationMethod and apparatus for sealing an opening in tissue of a living being
US4869143A (en)1985-06-111989-09-26Merrick Industries, Inc.Card file punch
US4890612A (en)1987-02-171990-01-02Kensey Nash CorporationDevice for sealing percutaneous puncture in a vessel
US4900303A (en)1978-03-101990-02-13Lemelson Jerome HDispensing catheter and method
US4920158A (en)*1989-10-111990-04-24Medipro Sciences LimitedHydrogel-forming wound dressing or skin coating material
US4929246A (en)1988-10-271990-05-29C. R. Bard, Inc.Method for closing and sealing an artery after removing a catheter
US4936835A (en)1988-05-261990-06-26Haaga John RMedical needle with bioabsorbable tip
JPH02182259A (en)*1989-01-061990-07-16Ube Ind LtdHemostatic sticking plaster
US4950234A (en)1987-05-261990-08-21Sumitomo Pharmaceuticals Company, LimitedDevice for administering solid preparations
US5007895A (en)1989-04-051991-04-16Burnett George SWound packing instrument
US5021059A (en)1990-05-071991-06-04Kensey Nash CorporationPlug device with pulley for sealing punctures in tissue and methods of use
US5049138A (en)1989-11-131991-09-17Boston Scientific CorporationCatheter with dissolvable tip
US5053046A (en)1988-08-221991-10-01Woodrow W. JaneseDural sealing needle and method of use
US5061274A (en)1989-12-041991-10-29Kensey Nash CorporationPlug device for sealing openings and method of use
US5080655A (en)1988-05-261992-01-14Haaga John RMedical biopsy needle
EP0476178A1 (en)1990-09-211992-03-25Bioplex Medical B.V.Device for placing styptic material on perforated blood vessels
US5106376A (en)1989-07-071992-04-21B. Braun Melsungen AgAnaesthesia set
US5108421A (en)1990-10-011992-04-28Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5129889A (en)1987-11-031992-07-14Hahn John LSynthetic absorbable epidural catheter
US5160323A (en)1989-05-261992-11-03Andrew Daniel EMethod and system for inserting spinal catheters
US5163904A (en)1991-11-121992-11-17Merit Medical Systems, Inc.Syringe apparatus with attached pressure gauge
US5167624A (en)1990-11-091992-12-01Catheter Research, Inc.Embolus delivery system and method
US5192300A (en)1990-10-011993-03-09Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5192290A (en)1990-08-291993-03-09Applied Medical Resources, Inc.Embolectomy catheter
US5192301A (en)1989-01-171993-03-09Nippon Zeon Co., Ltd.Closing plug of a defect for medical use and a closing plug device utilizing it
US5195988A (en)1988-05-261993-03-23Haaga John RMedical needle with removable sheath
US5219899A (en)1989-04-221993-06-15Degussa AktiengesellschaftPasty dental material which is an organopolysilane filler combined with a polymerizable bonding agent
US5221259A (en)1990-12-271993-06-22Novoste CorporationWound treating device and method of using same
US5220926A (en)1992-07-131993-06-22Jones George TFinger mounted core biopsy guide
US5232453A (en)1989-07-141993-08-03E. R. Squibb & Sons, Inc.Catheter holder
EP0557963A1 (en)1992-02-241993-09-01United States Surgical CorporationResilient arm mesh deployer
US5242683A (en)1989-07-211993-09-07Nycomed Imaging AsContrast media comprising a paramagnetic agent and an iodinated agent for x-ray and mri
US5254105A (en)1988-05-261993-10-19Haaga John RSheath for wound closure caused by a medical tubular device
EP0568334A1 (en)*1992-05-011993-11-03Amgen Inc.Collagen-containing sponges as drug delivery for proteins
US5282827A (en)1991-11-081994-02-01Kensey Nash CorporationHemostatic puncture closure system and method of use
US5299581A (en)1990-07-051994-04-05Donnell John TIntravaginal device
US5310407A (en)1991-06-171994-05-10Datascope Investment Corp.Laparoscopic hemostat delivery system and method for using said system
US5320639A (en)1993-03-121994-06-14Meadox Medicals, Inc.Vascular plug delivery system
US5322515A (en)1993-03-151994-06-21Abbott LaboratoriesLuer adapter assembly for emergency syringe
US5325857A (en)1993-07-091994-07-05Hossein NabaiSkin biopsy device and method
US5334216A (en)1992-12-101994-08-02Howmedica Inc.Hemostatic plug
US5342388A (en)1993-03-251994-08-30Sonia TollerMethod and apparatus for sealing luminal tissue
US5350399A (en)1991-09-231994-09-27Jay ErlebacherPercutaneous arterial puncture seal device and insertion tool therefore
US5352211A (en)1993-07-111994-10-04Louisville LaboratoriesExternal stability device
US5366480A (en)1990-12-241994-11-22American Cyanamid CompanySynthetic elastomeric buttressing pledget
US5370656A (en)1993-02-261994-12-06Merocel CorporationThroat pack
US5383896A (en)1993-05-251995-01-24Gershony; GaryVascular sealing device
US5383899A (en)1993-09-281995-01-24Hammerslag; Julius G.Method of using a surface opening adhesive sealer
US5385550A (en)1994-03-291995-01-31Su; Chan-HoNeedle protective means for prevention against stab and virus infection
EP0637431A1 (en)1993-08-051995-02-08VODA, JanSuture device
US5388588A (en)1993-05-041995-02-14Nabai; HosseinBiopsy wound closure device and method
US5391183A (en)1990-09-211995-02-21Datascope Investment CorpDevice and method sealing puncture wounds
US5417699A (en)1992-12-101995-05-23Perclose IncorporatedDevice and method for the percutaneous suturing of a vascular puncture site
US5419765A (en)1990-12-271995-05-30Novoste CorporationWound treating device and method for treating wounds
US5431639A (en)1993-08-121995-07-11Boston Scientific CorporationTreating wounds caused by medical procedures
US5437292A (en)1993-11-191995-08-01Bioseal, LlcMethod for sealing blood vessel puncture sites
US5443481A (en)1992-07-271995-08-22Lee; Benjamin I.Methods and device for percutaneous sealing of arterial puncture sites
US5447502A (en)1988-05-261995-09-05Haaga; John R.Sheath for wound closure caused by a medical tubular device
US5458570A (en)1991-01-221995-10-17May, Jr.; James W.Absorbable catheter and method of using the same
US5462194A (en)1995-01-111995-10-31Candea Inc.Self-venting straw tip
US5486195A (en)1993-07-261996-01-23Myers; GeneMethod and apparatus for arteriotomy closure
US5490736A (en)1994-09-081996-02-13Habley Medical Technology CorporationStylus applicator for a rehydrated multi-constituent medication
US5507279A (en)1993-11-301996-04-16Fortune; John B.Retrograde endotracheal intubation kit
US5522840A (en)1992-11-231996-06-04Krajicek; MilanDevice for the non-surgical seal of the interstice in the wall of a vessel
US5522850A (en)1994-06-231996-06-04Incontrol, Inc.Defibrillation and method for cardioverting a heart and storing related activity data
US5526822A (en)1994-03-241996-06-18Biopsys Medical, Inc.Method and apparatus for automated biopsy and collection of soft tissue
US5527332A (en)1994-11-021996-06-18Mectra Labs, Inc.Tissue cutter for surgery
US5540715A (en)1992-07-161996-07-30Sherwood Medical CompanyDevice for sealing hemostatic incisions
US5542914A (en)1993-02-121996-08-06Kimberly-Clark CorporationEncapsulated tampon with an applicator
US5545178A (en)1994-04-291996-08-13Kensey Nash CorporationSystem for closing a percutaneous puncture formed by a trocar to prevent tissue at the puncture from herniating
US5545175A (en)1993-06-181996-08-13Leonard BloomDisposable quarded finger scalpel for inserting a line in a patent and lock off therefor
US5554108A (en)1991-11-061996-09-10Tambrands Inc.Sanitary tampon
US5558853A (en)1993-01-251996-09-24Sonus PharmaceuticalsPhase shift colloids as ultrasound contrast agents
US5571168A (en)1995-04-051996-11-05Scimed Lifesystems IncPull back stent delivery system
US5595735A (en)*1990-05-231997-01-21Johnson & Johnson Medical, Inc.Hemostatic thrombin paste composition
US5601603A (en)1993-06-161997-02-11White Spot AgUse of and process for the introduction of fibrin sealant into a puncture channel
US5601601A (en)1991-12-131997-02-11Unisurge Holdings, Inc.Hand held surgical device
US5601207A (en)1996-03-131997-02-11Paczonay; Joseph R.Bite valve having a plurality of slits
US5620461A (en)1989-05-291997-04-15Muijs Van De Moer; Wouter M.Sealing device
US5645849A (en)1993-11-031997-07-08Clarion Pharmaceuticals, Inc.Hemostatic patch
US5645566A (en)1995-09-151997-07-08Sub Q Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US5649547A (en)1994-03-241997-07-22Biopsys Medical, Inc.Methods and devices for automated biopsy and collection of soft tissue
US5653730A (en)1993-09-281997-08-05Hemodynamics, Inc.Surface opening adhesive sealer
EP0637432B1 (en)1993-08-031997-10-01Aesculap AgLooping instrument
US5674346A (en)1992-12-151997-10-07Johnson & Johnson Consumer Products, Inc.Hydrogel laminate, bandages and composites and methods for forming the same
US5676689A (en)1991-11-081997-10-14Kensey Nash CorporationHemostatic puncture closure system including vessel location device and method of use
US5681279A (en)1996-11-041997-10-28Roper; David H.Pill dispensing syringe
US5769086A (en)1995-12-061998-06-23Biopsys Medical, Inc.Control system and method for automated biopsy device
US5782861A (en)1996-12-231998-07-21Sub Q Inc.Percutaneous hemostasis device
US5800389A (en)1996-02-091998-09-01Emx, Inc.Biopsy device
US5810806A (en)1996-08-291998-09-22Ethicon Endo-SurgeryMethods and devices for collection of soft tissue
US5827218A (en)1996-04-181998-10-27Stryker CorporationSurgical suction pool tip
US5858008A (en)1997-04-221999-01-12Becton, Dickinson And CompanyCannula sealing shield assembly
US5868762A (en)1997-09-251999-02-09Sub-Q, Inc.Percutaneous hemostatic suturing device and method
US5902310A (en)1996-08-121999-05-11Ethicon Endo-Surgery, Inc.Apparatus and method for marking tissue
US5931165A (en)1994-09-061999-08-03Fusion Medical Technologies, Inc.Films having improved characteristics and methods for their preparation and use
US6027471A (en)1995-01-182000-02-22Fallon; Timothy J.Apparatus for applying a hemostatic agent onto a tissue
US6027482A (en)1994-12-122000-02-22Becton Dickinson And CompanySyringe tip cap
US6033427A (en)1998-01-072000-03-07Lee; Benjamin I.Method and device for percutaneous sealing of internal puncture sites
US6056768A (en)1992-01-072000-05-02Cates; Christopher U.Blood vessel sealing system
US6063061A (en)*1996-08-272000-05-16Fusion Medical Technologies, Inc.Fragmented polymeric compositions and methods for their use
US6066325A (en)1996-08-272000-05-23Fusion Medical Technologies, Inc.Fragmented polymeric compositions and methods for their use
US6071301A (en)1998-05-012000-06-06Sub Q., Inc.Device and method for facilitating hemostasis of a biopsy tract
US6071300A (en)1995-09-152000-06-06Sub-Q Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US6126675A (en)1999-01-112000-10-03Ethicon, Inc.Bioabsorbable device and method for sealing vascular punctures
US6161034A (en)1999-02-022000-12-12Senorx, Inc.Methods and chemical preparations for time-limited marking of biopsy sites
US6162192A (en)*1998-05-012000-12-19Sub Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6183497B1 (en)1998-05-012001-02-06Sub-Q, Inc.Absorbable sponge with contrasting agent
US6197327B1 (en)1997-06-112001-03-06Umd, Inc.Device and method for treatment of dysmenorrhea
US6200328B1 (en)1998-05-012001-03-13Sub Q, IncorporatedDevice and method for facilitating hemostasis of a biopsy tract
US6315753B1 (en)1998-05-012001-11-13Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US20020002889A1 (en)2000-04-282002-01-10Mark AshbyEasy cutter
US20020016612A1 (en)1998-05-012002-02-07Mark AshbyDevice and method for facilitating hemostasis of a biopsy tract
US20020042378A1 (en)*1999-06-102002-04-11Cary J. ReichHemoactive compositions and methods for their manufacture and use
US20020062104A1 (en)1999-09-232002-05-23Mark AshbyDepth and puncture control for blood vessel hemostasis system
US6503222B2 (en)2000-09-282003-01-07Pfizer IncOral dosage dispenser
US20030028140A1 (en)2001-03-122003-02-06Greff Richard J.Cross-linked gelatin composition comprising a wetting agent
US6540735B1 (en)2000-05-122003-04-01Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6544236B1 (en)1999-02-102003-04-08Sub-Q, IncorporatedDevice, system and method for improving delivery of hemostatic material
US6547806B1 (en)2000-02-042003-04-15Ni DingVascular sealing device and method of use
US20030088269A1 (en)2001-11-082003-05-08Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US6585680B2 (en)1999-11-292003-07-01Scan-Mark, Inc.Suction tube for surgical purposes
US6610026B2 (en)1998-05-012003-08-26Sub-Q, Inc.Method of hydrating a sponge material for delivery to a body
US20040019328A1 (en)2001-11-082004-01-29Sing Eduardo ChiSystem and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US20040019330A1 (en)2001-11-082004-01-29Sub-Q, Inc., A California CorporationSheath based blood vessel puncture locator and depth indicator

Family Cites Families (26)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US3325366A (en)*1964-11-091967-06-13Seymour M BlaugBiologically absorbable foam packing bandage and process therefor
SU782814A1 (en)1977-01-181980-11-30За вительProsthesis for closing defect in heart tissues
SU1088709A1 (en)1981-02-101984-04-30Институт Клинической И Экспериментальной ХирургииMethod of treatment of stomach fistula
US4696812A (en)*1985-10-281987-09-29Warner-Lambert CompanyThrombin preparations
US5092873A (en)1990-02-281992-03-03Devices For Vascular Intervention, Inc.Balloon configuration for atherectomy catheter
WO1994028800A1 (en)1993-06-041994-12-22Kensey Nash CorporationHemostatic vessel puncture closure with filament lock
AU1999995A (en)1994-04-081995-11-10Atrix Laboratories, Inc.An adjunctive polymer system for use with medical device
US5554029A (en)1994-05-311996-09-10Medical Laser Technology, Inc.Dental laser apparatus and method for ablating non-metallic dental material from a tooth
WO1995032671A1 (en)1994-06-011995-12-07Perclose, Inc.Method and device for providing vascular hemostasis
WO1995032669A1 (en)1994-06-011995-12-07Perclose, Inc.Apparatus and method for advancing surgical knots
JPH10508504A (en)1994-09-161998-08-25バイオプシス メディカル インコーポレイテッド Method and apparatus for identifying and marking tissue
US5660854A (en)*1994-11-281997-08-26Haynes; Duncan HDrug releasing surgical implant or dressing material
US5649959A (en)1995-02-101997-07-22Sherwood Medical CompanyAssembly for sealing a puncture in a vessel
US6270464B1 (en)1998-06-222001-08-07Artemis Medical, Inc.Biopsy localization method and device
US20020076429A1 (en)*1998-01-282002-06-20John F. WironenBone paste subjected to irradiative and thermal treatment
US7625352B1 (en)1998-05-012009-12-01Sub-Q, Inc.Depth and puncture control for system for hemostasis of blood vessel
US7695492B1 (en)1999-09-232010-04-13Boston Scientific Scimed, Inc.Enhanced bleed back system
US20020022822A1 (en)2000-07-142002-02-21Cragg Andrew H.Sheath-mounted arterial plug delivery device
US7201725B1 (en)2000-09-252007-04-10Sub-Q, Inc.Device and method for determining a depth of an incision
US7029489B1 (en)2001-05-182006-04-18Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture site
US7037323B2 (en)2001-11-082006-05-02Sub-Q, Inc.Pledget-handling system and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US7037322B1 (en)2001-11-082006-05-02Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture with a staging tube
US20040102730A1 (en)2002-10-222004-05-27Davis Thomas P.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US8317821B1 (en)2002-11-042012-11-27Boston Scientific Scimed, Inc.Release mechanism
US7455680B1 (en)2002-11-042008-11-25Boston Scientific Scimed, Inc.Apparatus and method for inhibiting blood loss
US7955353B1 (en)2002-11-042011-06-07Sub-Q, Inc.Dissolvable closure device

Patent Citations (215)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US581235A (en)1897-04-20Island
US2899362A (en)1959-08-11Hemostatic sponges and method of
US1578517A (en)1924-12-231926-03-30George N HeinValve piston and barrel construction for hypodermic syringes
US2086580A (en)1935-06-241937-07-13Myron C ShirleyApplicator
US2465357A (en)1944-08-141949-03-29Upjohn CoTherapeutic sponge and method of making
US2370319A (en)1944-11-071945-02-27Dohner & LippincottPaper perforator
US2492458A (en)1944-12-081949-12-27Jr Edgar A BeringFibrin foam
US2507244A (en)1947-04-141950-05-09Upjohn CoSurgical gelatin dusting powder and process for preparing same
US2558395A (en)1947-06-031951-06-26Hoffmann La RocheUndenatured gelatin hemostatic sponge containing thrombin
US2597011A (en)1950-07-281952-05-20Us AgriculturePreparation of starch sponge
US2680442A (en)1952-04-041954-06-08Frank L LinzmayerDisposable suppository casing
US2814294A (en)1953-04-171957-11-26Becton Dickinson CoUnit for and method of inhibiting and controlling bleeding tendencies
US2874776A (en)1954-06-071959-02-24Royal Mcbee CorpPunch and die mechanism
US2824092A (en)1955-01-041958-02-18Robert E ThompsonProcess of preparation of a gelatincarboxymethyl cellulose complex
US2761446A (en)1955-03-301956-09-04Chemical Specialties Co IncImplanter and cartridge
US2997195A (en)1959-07-161961-08-22Yuen Yat ChuenDrinking straws
US3157524A (en)1960-10-251964-11-17Ethicon IncPreparation of collagen sponge
US3358689A (en)1964-06-091967-12-19Roehr Products Company IncIntegral lancet and package
US3411505A (en)1965-12-151968-11-19Paul D. NobisDevice for interrupting arterial flow
US3703174A (en)1970-07-141972-11-21Medidyne CorpMethod and apparatus for catheter injection
US3724465A (en)1971-07-221973-04-03Kimberly Clark CoTampon coated with insertion aid and method for coating
US3736939A (en)1972-01-071973-06-05Kendall & CoBalloon catheter with soluble tip
GB1509023A (en)1973-02-121978-04-26Ochsner Med Found AltonSeptal defect closure apparatus
US4000741A (en)1975-11-031977-01-04The Kendall CompanySyringe assembly
US4098728A (en)1976-01-021978-07-04Solomon RosenblattMedical surgical sponge and method of making same
GB1569660A (en)1976-07-301980-06-18Medline AbOcclusion of body channels
US4218155A (en)1978-02-101980-08-19Etablissements Armor, S.A.Stick for applying a liquid
US4900303A (en)1978-03-101990-02-13Lemelson Jerome HDispensing catheter and method
US4588395A (en)1978-03-101986-05-13Lemelson Jerome HCatheter and method
US4404970A (en)1978-05-191983-09-20Sawyer Philip NicholasHemostatic article and methods for preparing and employing the same
US4238480A (en)1978-05-191980-12-09Sawyer Philip NicholasMethod for preparing an improved hemostatic agent and method of employing the same
US4224945A (en)1978-08-301980-09-30Jonathan CohenInflatable expansible surgical pressure dressing
US4219026A (en)1978-09-151980-08-26The Kendall CompanyBladder hemostatic catheter
US4211323A (en)1978-12-011980-07-08California Medical Developments, Inc.Disposable diagnostic swab having a stored culture medium
EP0032826B1 (en)1980-01-181984-06-20Shiley IncorporatedVein distention apparatus
US4323072A (en)1980-01-181982-04-06Shiley, IncorporatedCannula for a vein distention system
US4340066A (en)1980-02-011982-07-20Sherwood Medical Industries Inc.Medical device for collecting a body sample
US4292972A (en)1980-07-091981-10-06E. R. Squibb & Sons, Inc.Lyophilized hydrocolloio foam
US4390018A (en)1980-09-151983-06-28Zukowski Henry JMethod for preventing loss of spinal fluid after spinal tap
US4405314A (en)1982-04-191983-09-20Cook IncorporatedApparatus and method for catheterization permitting use of a smaller gage needle
US4645488A (en)1982-08-121987-02-24Board Of Trustees Of The University Of AlabamaSyringe for extrusion of wetted, particulate material
US4591094A (en)1983-08-131986-05-27Arthur MorrisFountain
US4573576A (en)1983-10-271986-03-04Krol Thomas CPercutaneous gastrostomy kit
US4515637A (en)1983-11-161985-05-07Seton CompanyCollagen-thrombin compositions
US4619913A (en)1984-05-291986-10-28Matrix Pharmaceuticals, Inc.Treatments employing drug-containing matrices for introduction into cellular lesion areas
US4619261A (en)1984-08-091986-10-28Frederico GuerrieroHydrostatic pressure device for bleeding control through an inflatable, stitchable and retrievable balloon-net system
US4587969A (en)1985-01-281986-05-13Rolando GillisSupport assembly for a blood vessel or like organ
US4869143A (en)1985-06-111989-09-26Merrick Industries, Inc.Card file punch
US4708718A (en)1985-07-021987-11-24Target TherapeuticsHyperthermic treatment of tumors
US4644649A (en)1985-09-261987-02-24Seaman Roy CApparatus for trimming reeds of musical instruments
US4832688A (en)1986-04-091989-05-23Terumo Kabushiki KaishaCatheter for repair of blood vessel
US4699616A (en)1986-06-131987-10-13Hollister IncorporatedCatheter retention device and method
US4744364A (en)1987-02-171988-05-17Intravascular Surgical Instruments, Inc.Device for sealing percutaneous puncture in a vessel
US4890612A (en)1987-02-171990-01-02Kensey Nash CorporationDevice for sealing percutaneous puncture in a vessel
US4852568A (en)1987-02-171989-08-01Kensey Nash CorporationMethod and apparatus for sealing an opening in tissue of a living being
US4839204A (en)1987-05-191989-06-13Yazaki Kakoh Co., Ltd.Resin coated metal pipe having a plane surface for a lightweight structure
US4950234A (en)1987-05-261990-08-21Sumitomo Pharmaceuticals Company, LimitedDevice for administering solid preparations
US4829994A (en)1987-05-271989-05-16Kurth Paul AFemoral compression device for post-catheterization hemostasis
US4836204A (en)1987-07-061989-06-06Landymore Roderick WMethod for effecting closure of a perforation in the septum of the heart
US4850960A (en)1987-07-081989-07-25Joseph GrayzelDiagonally tapered, bevelled tip introducing catheter and sheath and method for insertion
US4790819A (en)1987-08-241988-12-13American Cyanamid CompanyFibrin clot delivery device and method
US5129889A (en)1987-11-031992-07-14Hahn John LSynthetic absorbable epidural catheter
US5447502A (en)1988-05-261995-09-05Haaga; John R.Sheath for wound closure caused by a medical tubular device
US5080655A (en)1988-05-261992-01-14Haaga John RMedical biopsy needle
US5254105A (en)1988-05-261993-10-19Haaga John RSheath for wound closure caused by a medical tubular device
US5195988A (en)1988-05-261993-03-23Haaga John RMedical needle with removable sheath
US4936835A (en)1988-05-261990-06-26Haaga John RMedical needle with bioabsorbable tip
US5053046A (en)1988-08-221991-10-01Woodrow W. JaneseDural sealing needle and method of use
US4929246A (en)1988-10-271990-05-29C. R. Bard, Inc.Method for closing and sealing an artery after removing a catheter
JPH02182259A (en)*1989-01-061990-07-16Ube Ind LtdHemostatic sticking plaster
FR2641692B1 (en)1989-01-171995-05-12Nippon Zeon Co
US5192301A (en)1989-01-171993-03-09Nippon Zeon Co., Ltd.Closing plug of a defect for medical use and a closing plug device utilizing it
US5007895A (en)1989-04-051991-04-16Burnett George SWound packing instrument
US5219899A (en)1989-04-221993-06-15Degussa AktiengesellschaftPasty dental material which is an organopolysilane filler combined with a polymerizable bonding agent
US5160323A (en)1989-05-261992-11-03Andrew Daniel EMethod and system for inserting spinal catheters
US5620461A (en)1989-05-291997-04-15Muijs Van De Moer; Wouter M.Sealing device
US5106376A (en)1989-07-071992-04-21B. Braun Melsungen AgAnaesthesia set
US5232453A (en)1989-07-141993-08-03E. R. Squibb & Sons, Inc.Catheter holder
US5242683A (en)1989-07-211993-09-07Nycomed Imaging AsContrast media comprising a paramagnetic agent and an iodinated agent for x-ray and mri
US4920158A (en)*1989-10-111990-04-24Medipro Sciences LimitedHydrogel-forming wound dressing or skin coating material
US5049138A (en)1989-11-131991-09-17Boston Scientific CorporationCatheter with dissolvable tip
US5061274A (en)1989-12-041991-10-29Kensey Nash CorporationPlug device for sealing openings and method of use
US5021059A (en)1990-05-071991-06-04Kensey Nash CorporationPlug device with pulley for sealing punctures in tissue and methods of use
US5595735A (en)*1990-05-231997-01-21Johnson & Johnson Medical, Inc.Hemostatic thrombin paste composition
US5299581A (en)1990-07-051994-04-05Donnell John TIntravaginal device
US5192290A (en)1990-08-291993-03-09Applied Medical Resources, Inc.Embolectomy catheter
US5741223A (en)1990-09-211998-04-21Datascope Investment Corp.Device and method for sealing puncture wounds
EP0482350B1 (en)1990-09-211996-12-27Datascope Investment Corp.Device for sealing puncture wounds
US5391183A (en)1990-09-211995-02-21Datascope Investment CorpDevice and method sealing puncture wounds
US5591204A (en)1990-09-211997-01-07Datascope Investment Corp.Device and method for sealing puncture wounds
US5437631A (en)1990-09-211995-08-01Datascope Investment Corp.Percutaneous introducer set and method for sealing puncture wounds
US5830130A (en)1990-09-211998-11-03Datascope Investment Corp.Device and method for sealing puncture wounds
EP0476178A1 (en)1990-09-211992-03-25Bioplex Medical B.V.Device for placing styptic material on perforated blood vessels
US5725498A (en)1990-09-211998-03-10Datascope Investment Corp.Device and method for sealing puncture wounds
US5275616B1 (en)1990-10-011996-01-23Quinton InstrInsertion assembly and method of inserting a vessel plug into the body of a patient
US5478352A (en)1990-10-011995-12-26Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5601602A (en)1990-10-011997-02-11Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5716375A (en)1990-10-011998-02-10Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5108421A (en)1990-10-011992-04-28Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5275616A (en)1990-10-011994-01-04Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5591205A (en)1990-10-011997-01-07Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5192300A (en)1990-10-011993-03-09Quinton Instrument CompanyInsertion assembly and method of inserting a vessel plug into the body of a patient
US5167624A (en)1990-11-091992-12-01Catheter Research, Inc.Embolus delivery system and method
US5366480A (en)1990-12-241994-11-22American Cyanamid CompanySynthetic elastomeric buttressing pledget
US5221259A (en)1990-12-271993-06-22Novoste CorporationWound treating device and method of using same
US5419765A (en)1990-12-271995-05-30Novoste CorporationWound treating device and method for treating wounds
US5458570A (en)1991-01-221995-10-17May, Jr.; James W.Absorbable catheter and method of using the same
US5310407A (en)1991-06-171994-05-10Datascope Investment Corp.Laparoscopic hemostat delivery system and method for using said system
US5350399A (en)1991-09-231994-09-27Jay ErlebacherPercutaneous arterial puncture seal device and insertion tool therefore
US5554108A (en)1991-11-061996-09-10Tambrands Inc.Sanitary tampon
US5707393A (en)1991-11-081998-01-13Kensey Nash CorporationHemostatic puncture closure system and method of use
US5282827A (en)1991-11-081994-02-01Kensey Nash CorporationHemostatic puncture closure system and method of use
US6090130A (en)1991-11-082000-07-18Kensey Nash CorporationHemostatic puncture closure system including blood vessel locator and method of use
US5676689A (en)1991-11-081997-10-14Kensey Nash CorporationHemostatic puncture closure system including vessel location device and method of use
US6007563A (en)1991-11-081999-12-28Kensey Nash CorporationMethod of deploying percutaneous puncture closure
US5163904A (en)1991-11-121992-11-17Merit Medical Systems, Inc.Syringe apparatus with attached pressure gauge
US5601601A (en)1991-12-131997-02-11Unisurge Holdings, Inc.Hand held surgical device
US6056768A (en)1992-01-072000-05-02Cates; Christopher U.Blood vessel sealing system
EP0557963A1 (en)1992-02-241993-09-01United States Surgical CorporationResilient arm mesh deployer
EP0568334A1 (en)*1992-05-011993-11-03Amgen Inc.Collagen-containing sponges as drug delivery for proteins
US5399361A (en)1992-05-011995-03-21Amgen Inc.Collagen-containing sponges as drug delivery compositions for proteins
US5220926A (en)1992-07-131993-06-22Jones George TFinger mounted core biopsy guide
US5540715A (en)1992-07-161996-07-30Sherwood Medical CompanyDevice for sealing hemostatic incisions
US5443481A (en)1992-07-271995-08-22Lee; Benjamin I.Methods and device for percutaneous sealing of arterial puncture sites
US5522840A (en)1992-11-231996-06-04Krajicek; MilanDevice for the non-surgical seal of the interstice in the wall of a vessel
US5417699A (en)1992-12-101995-05-23Perclose IncorporatedDevice and method for the percutaneous suturing of a vascular puncture site
US5334216A (en)1992-12-101994-08-02Howmedica Inc.Hemostatic plug
US5674346A (en)1992-12-151997-10-07Johnson & Johnson Consumer Products, Inc.Hydrogel laminate, bandages and composites and methods for forming the same
US5558853A (en)1993-01-251996-09-24Sonus PharmaceuticalsPhase shift colloids as ultrasound contrast agents
US5542914A (en)1993-02-121996-08-06Kimberly-Clark CorporationEncapsulated tampon with an applicator
US5370656A (en)1993-02-261994-12-06Merocel CorporationThroat pack
US5320639A (en)1993-03-121994-06-14Meadox Medicals, Inc.Vascular plug delivery system
US5322515A (en)1993-03-151994-06-21Abbott LaboratoriesLuer adapter assembly for emergency syringe
US5342388A (en)1993-03-251994-08-30Sonia TollerMethod and apparatus for sealing luminal tissue
US5388588A (en)1993-05-041995-02-14Nabai; HosseinBiopsy wound closure device and method
US5467780A (en)1993-05-041995-11-21Nabai; HosseinBiopsy wound closure device and method
US5479936A (en)1993-05-041996-01-02Nabai; HosseinBiopsy wound closure device and method
US5383896A (en)1993-05-251995-01-24Gershony; GaryVascular sealing device
US5601603A (en)1993-06-161997-02-11White Spot AgUse of and process for the introduction of fibrin sealant into a puncture channel
US5545175A (en)1993-06-181996-08-13Leonard BloomDisposable quarded finger scalpel for inserting a line in a patent and lock off therefor
US5325857A (en)1993-07-091994-07-05Hossein NabaiSkin biopsy device and method
US5352211A (en)1993-07-111994-10-04Louisville LaboratoriesExternal stability device
US5486195A (en)1993-07-261996-01-23Myers; GeneMethod and apparatus for arteriotomy closure
EP0637432B1 (en)1993-08-031997-10-01Aesculap AgLooping instrument
EP0637431A1 (en)1993-08-051995-02-08VODA, JanSuture device
US5431639A (en)1993-08-121995-07-11Boston Scientific CorporationTreating wounds caused by medical procedures
US5665107A (en)1993-09-281997-09-09Hemodynamics, Inc.Surface opening adhesive sealer
US5529577A (en)1993-09-281996-06-25Hemodynamics, Inc.Surface opening adhesive sealer
US5383899A (en)1993-09-281995-01-24Hammerslag; Julius G.Method of using a surface opening adhesive sealer
US5653730A (en)1993-09-281997-08-05Hemodynamics, Inc.Surface opening adhesive sealer
US5645849A (en)1993-11-031997-07-08Clarion Pharmaceuticals, Inc.Hemostatic patch
US5437292A (en)1993-11-191995-08-01Bioseal, LlcMethod for sealing blood vessel puncture sites
US5507279A (en)1993-11-301996-04-16Fortune; John B.Retrograde endotracheal intubation kit
US5526822A (en)1994-03-241996-06-18Biopsys Medical, Inc.Method and apparatus for automated biopsy and collection of soft tissue
US5649547A (en)1994-03-241997-07-22Biopsys Medical, Inc.Methods and devices for automated biopsy and collection of soft tissue
US5775333A (en)1994-03-241998-07-07Ethicon Endo-Surgery, Inc.Apparatus for automated biopsy and collection of soft tissue
US5385550A (en)1994-03-291995-01-31Su; Chan-HoNeedle protective means for prevention against stab and virus infection
US5545178A (en)1994-04-291996-08-13Kensey Nash CorporationSystem for closing a percutaneous puncture formed by a trocar to prevent tissue at the puncture from herniating
US5522850A (en)1994-06-231996-06-04Incontrol, Inc.Defibrillation and method for cardioverting a heart and storing related activity data
US5931165A (en)1994-09-061999-08-03Fusion Medical Technologies, Inc.Films having improved characteristics and methods for their preparation and use
US5490736A (en)1994-09-081996-02-13Habley Medical Technology CorporationStylus applicator for a rehydrated multi-constituent medication
US5527332A (en)1994-11-021996-06-18Mectra Labs, Inc.Tissue cutter for surgery
US6027482A (en)1994-12-122000-02-22Becton Dickinson And CompanySyringe tip cap
US5462194A (en)1995-01-111995-10-31Candea Inc.Self-venting straw tip
US6027471A (en)1995-01-182000-02-22Fallon; Timothy J.Apparatus for applying a hemostatic agent onto a tissue
US5571168A (en)1995-04-051996-11-05Scimed Lifesystems IncPull back stent delivery system
US6071300A (en)1995-09-152000-06-06Sub-Q Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US20020156495A1 (en)1995-09-152002-10-24Rodney BrennemanApparatus and method for percutaneous sealing of blood vessel punctures
US6371974B1 (en)1995-09-152002-04-16Sub Q, Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US5645566A (en)1995-09-151997-07-08Sub Q Inc.Apparatus and method for percutaneous sealing of blood vessel punctures
US5769086A (en)1995-12-061998-06-23Biopsys Medical, Inc.Control system and method for automated biopsy device
US5800389A (en)1996-02-091998-09-01Emx, Inc.Biopsy device
US5601207A (en)1996-03-131997-02-11Paczonay; Joseph R.Bite valve having a plurality of slits
US5827218A (en)1996-04-181998-10-27Stryker CorporationSurgical suction pool tip
US5902310A (en)1996-08-121999-05-11Ethicon Endo-Surgery, Inc.Apparatus and method for marking tissue
US6066325A (en)1996-08-272000-05-23Fusion Medical Technologies, Inc.Fragmented polymeric compositions and methods for their use
US6063061A (en)*1996-08-272000-05-16Fusion Medical Technologies, Inc.Fragmented polymeric compositions and methods for their use
US5810806A (en)1996-08-291998-09-22Ethicon Endo-SurgeryMethods and devices for collection of soft tissue
US5681279A (en)1996-11-041997-10-28Roper; David H.Pill dispensing syringe
US5984950A (en)1996-12-231999-11-16Sub-Q, Inc.Percutaneous hemostasis device
US5782861A (en)1996-12-231998-07-21Sub Q Inc.Percutaneous hemostasis device
US5858008A (en)1997-04-221999-01-12Becton, Dickinson And CompanyCannula sealing shield assembly
US6197327B1 (en)1997-06-112001-03-06Umd, Inc.Device and method for treatment of dysmenorrhea
US5868762A (en)1997-09-251999-02-09Sub-Q, Inc.Percutaneous hemostatic suturing device and method
US6033427A (en)1998-01-072000-03-07Lee; Benjamin I.Method and device for percutaneous sealing of internal puncture sites
US6071301A (en)1998-05-012000-06-06Sub Q., Inc.Device and method for facilitating hemostasis of a biopsy tract
US6086607A (en)1998-05-012000-07-11Sub-Q, Inc.Device and method for facilitating hemostasis of a biopsy tract
US6183497B1 (en)1998-05-012001-02-06Sub-Q, Inc.Absorbable sponge with contrasting agent
US6610026B2 (en)1998-05-012003-08-26Sub-Q, Inc.Method of hydrating a sponge material for delivery to a body
US6200328B1 (en)1998-05-012001-03-13Sub Q, IncorporatedDevice and method for facilitating hemostasis of a biopsy tract
US6315753B1 (en)1998-05-012001-11-13Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US20030135237A1 (en)1998-05-012003-07-17Cragg Andrew H.Device, system and method for improving delivery of hemostatic material
US20020016612A1 (en)1998-05-012002-02-07Mark AshbyDevice and method for facilitating hemostasis of a biopsy tract
US20020038133A1 (en)1998-05-012002-03-28Sing Eduardo ChiAbsorbable sponge with contrasting agent
US20030088271A1 (en)*1998-05-012003-05-08Cragg Andrew M.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6527734B2 (en)1998-05-012003-03-04Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6162192A (en)*1998-05-012000-12-19Sub Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6440153B2 (en)1998-05-012002-08-27Sub-Q, Inc.Device and method for facilitating hemostasis of a biopsy tract
US6440151B1 (en)1998-05-012002-08-27Sub-Q, Inc.Device and method for facilitating hemostasis of a biopsy tract
US6447534B2 (en)1998-05-012002-09-10Sub-Q, Inc.Device and method for facilitating hemostasis of a biopsy tract
US6126675A (en)1999-01-112000-10-03Ethicon, Inc.Bioabsorbable device and method for sealing vascular punctures
US6161034A (en)1999-02-022000-12-12Senorx, Inc.Methods and chemical preparations for time-limited marking of biopsy sites
US6544236B1 (en)1999-02-102003-04-08Sub-Q, IncorporatedDevice, system and method for improving delivery of hemostatic material
US20020042378A1 (en)*1999-06-102002-04-11Cary J. ReichHemoactive compositions and methods for their manufacture and use
US20020062104A1 (en)1999-09-232002-05-23Mark AshbyDepth and puncture control for blood vessel hemostasis system
US6585680B2 (en)1999-11-292003-07-01Scan-Mark, Inc.Suction tube for surgical purposes
US6547806B1 (en)2000-02-042003-04-15Ni DingVascular sealing device and method of use
US20020002889A1 (en)2000-04-282002-01-10Mark AshbyEasy cutter
US6540735B1 (en)2000-05-122003-04-01Sub-Q, Inc.System and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US20030120258A1 (en)2000-05-122003-06-26Mark AshbySystem and method for facilitating hemostasis of blood vessel punctures with absorbable sponge
US6503222B2 (en)2000-09-282003-01-07Pfizer IncOral dosage dispenser
US20030028140A1 (en)2001-03-122003-02-06Greff Richard J.Cross-linked gelatin composition comprising a wetting agent
US20030088269A1 (en)2001-11-082003-05-08Sub-Q, Inc.System and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US20040019328A1 (en)2001-11-082004-01-29Sing Eduardo ChiSystem and method for delivering hemostasis promoting material to a blood vessel puncture site by fluid pressure
US20040019330A1 (en)2001-11-082004-01-29Sub-Q, Inc., A California CorporationSheath based blood vessel puncture locator and depth indicator

Non-Patent Citations (50)

* Cited by examiner, † Cited by third party
Title
(125) Ashby, Mark et al; U.S. Appl. No. 10/287,922; filed Nov. 4, 2002; entitled: Apparatus and Method for Inhibiting Blood Loss.
(130) Ashby, Mark et al; U.S. Appl. No. 10/069,107, filed Dec. 16, 2002; entitled: Device and Method for Determining a Depth of an Incision.
(144) Ashby, Mark et al; U.S. Appl. No. 10/278,710, filed Oct. 22, 2002; entitled: "System and Method for Facilitating Hemostasis of Blood Vessel Punctures With Absorbable Sponge".
(152) Ashby, Mark et al; U.S. Appl. No. 10/334,770, filed Dec 31, 2002; entitled: "Improved System and Method for Facilitating Hemostasis with Absorbable Sponge".
(154) Ashby, Mark et al; U.S. Appl. No. 10/421,680, filed Apr. 22, 2003; entitled: "Puncture Closure System With Pin and Pull Technique".
(159) Ashby, Mark et al; U.S. Appl. No. 10/462,065, filed Jun. 12, 2003; entitled: "Enhanced Bleed Back System".
(160) Ashby, Mark et al, U.S. Appl. No. 10/462,064, filed Jun. 12, 2003; entitled: "Release Mechanism".
(161) Ashby, Mark et al; U.S. Appl. No. 10/461,587, filed Jun. 12, 2003; entitled: "Dissolvable Closure Device".
(162) Ashby, Mark et al; U.S. Appl. No. 10/461,035, filed Jun. 13, 2003; entitled: "System and Method for Delivering Hemostasis Promoting Material to a Blood Vessel Puncture Site Using a Cannula".
(163) Ashby, Mark et al; U.S. Appl. No. 10/461,006, filed Jun. 13, 2003; entitled: "System and Method for Delivering Hemostasis Promoting Material to a Blood Vessel Puncture with a Staging Tube".
(164) Ashby, Mark et al; U.S. Appl. No. 10/460,859, filed Jun. 12, 2003; entitled: "Hemostatic Device Including a Capsule".
(187) Ashby, Mark et al; U.S. Appl. No. 10/732,441, filed Dec. 9, 2003; entitled: "Pledget-Handling System and Method for Delivering Hemostasis Promoting Material to a Blood Vessel Puncture Site by Fluid Pressure".
(190) Ashby, Mark et al; U.S. Appl. No. 10/754,824, filed Jan. 9, 2004; entitled: "Sheath-Mounted Arterial Plug Delivery Device".
Allison, D., et al., "Percutaneous liver biopsy and track embolization with steel coils", Radiology, vol. 169, pp. 261-263, (1998).
Berman et al "Modification of the Cope Drainage Catheter to Facilitate Placement" AJR 146:169-170, 1/86 0361-803X/86/1461-0169 © American Ray Society.
Berman, Howard L., et al, "Guided Direct Antegrade Puncture of the Superficial Femoral Artry," American Roantgen Ray Society, pp. 632-634 (Sep. 1986).
Chuang, V., et al., "Sheath needle for liver biopsy in high-risk patience", Radiology, vol. 166, pp. 261-262 (1988).
Correll, et al , Proc. Soc. Exp. Biol. N.Y., 58:233 (1945).
Correll, et al., Surg. Gyn. and Obst., 82:585 (1945).
Fandrich, C., et al. "Small guage gelfoam plug liver biopsy in high risk patients", Australian Radiology, vol. 40, pp. 230-234 (1996).
Foran, JPM, et al. "Early mobilisation after percutaneous cardiac catheterisation using collagen plug (vasoseal) maemostatis" BRHeart, vol. 69, pp. 424-429 (1993).
Gibbs, JSR, "Femoral arterial hemostasis" J. Interventional card, vol. 5, pp. 85-88 (1992).
J. Bryne Review Article: Endovascular treatments for intracranial anuerysms, 1996 The British journal of radiology; 98,891-899.
John T. Correll, et al. Biologic investigations of new absorbable sponge; p. 585 , 1945.
John T. Correll, et al., A new Physiologically absorbable sponge , 1945.
Journal of interventional cardiology vol. 5 No. 2 Jun. 1992.
Kassel, et al. Size of Intracanial aneurysm; vol. 12, No. 3, (1983).
Kiemeneiji, F, et al., "Improved anticoagulation management after Palmaz Schatz coronary stent implantation by sealing the arterial puncture site with vascular hemostasis device", Catheterization and Cardiovascular diagnosis, vol. 30, pp. 1685-1692 (1995).
Kussmaul, WG, "Rapid arterial hemostasis", J. Am. Coll. Card., vol. 25, pp. 1685-1692 (1995).
Lim et al , "Barrier and Tensile Properties of Transglutaminase Cross-linked Gelatin Films as Affected by Relative Humidity, Temperature, and Glycerol Content," Journal of Food Science, vol. 64, NR. 4, pp. 616-622, XP009084131, (Jul. 1999).
PCT International Search Report.
Pharmacia & Upjohn manufacturer brochure "gelfoam sterile powder", (Feb. 1996).
Pharmacia & Upjohn manufacturer brochure (Sep. 1996).
Pharmacia & Upjohn manufacturer brochure gelfoam sterile sponge, sterile powder and sterile film, pp. 1-34 (May 1997).
Pharmacia & Upjohn manufacturer brochure, "gelfoam sterile powder" (Mar. 1996).
Pharmacia & Upjohn manufacturer specification, "Gelfoam sterile sponge, sterile powder and sterile film" pp. 1-23 (Nov. 1996).
Ricardo Di Segni et al. "Part 1. Embolotherapy: Agents, Equipment, and Techniques" Vascular Embolotherapy 4 , 1992.
Riley, SA, Percutaneous liver biopsy with plugging of needle track: a safe method for use in patients with impaired coagulation, The lancet, p. 436 (1964).
Sanborn, T. Multicenter randomized trial comparing perutaneous collagen hemostasis device with conventional manual compression after diagnostic angiography and angioplasty , J. Am. Coll. Card., vol. 22, pp. 1273-1279, (1993).
Scharader, R. "Collagen appl.", Catheterization & cardiovascular diagnosis (1992) pp. 298-302.
Schievink, et al. The new england journal of medicaine; review articles; intracanial aneurysms; Jan. 2, 1997.
Silber, S., "Rapid hemostasis of arterial puncture sites with collagen in patients undergoing diagnostic interventional cardiac catherterization", clinical cardiology, vol. 20, pp. 981-992, (1997).
Smith, T., "Percutaneous transhepatic liver biopsy with tract embolization", Radiology, vol. 198, pp. 769-774 (1996).
Supplementary Partial European Search Report EP 02 72 0915; report dated Jun. 11, 2007.
Szikora, et al. Combined Use of stents and cells to treat experimental wide-necked carotid aneuryms: Preliminary results; AJNR AM newradiol 15: 1091-1102, Jun. 94.
Szikora, et al. Endovascular treatment of experimental anuerysms with liquid polymers: vol. 38, No. 2, Feb. 96.
Turjman, et al. Combined stent implantation & endosacular coil placement for tretment of experimental wide-necked aneurysms:Ajnram J. Neuroradio 15: 1087-1090 Jun. 94.
Vogelzang, Robert L., "A Modified Cope Introducing Dilator to Allow Straight Guide Wire Introduction," American Roantigen Ray Society, pp. 381-382 (Feb. 1986).
Yoshimoto, et al cerebral anuerysms unrelated to arterial bifurcations; Acta neurochir (Wien) (96) 138: 958-964.
Zins, M., "US-guided percutaneous liver biopsy with plugging of the needle track" radiology, vol. 187, pp. 841-843, (1992).

Cited By (2)

* Cited by examiner, † Cited by third party
Publication numberPriority datePublication dateAssigneeTitle
US8821918B2 (en)2001-03-122014-09-02Boston Scientific Scimed Inc.Cross-linked gelatin composition comprising a wetting agent
US11679177B2 (en)2017-08-082023-06-20Baxter International Inc.Polymeric compositions, delivery devices, and methods

Also Published As

Publication numberPublication date
EP1389125B1 (en)2014-08-20
EP1389125A4 (en)2007-07-25
US20030028140A1 (en)2003-02-06
US8821918B2 (en)2014-09-02
EP1389125A1 (en)2004-02-18
US20130324470A1 (en)2013-12-05
WO2002072128A1 (en)2002-09-19
US8524270B2 (en)2013-09-03
US20120232013A1 (en)2012-09-13

Similar Documents

PublicationPublication DateTitle
US8187625B2 (en)Cross-linked gelatin composition comprising a wetting agent
US5595735A (en)Hemostatic thrombin paste composition
JP5232347B2 (en) Blood active compositions and methods for their manufacture and use
US10322170B2 (en)Hemostatic compositions
CA2851321C (en)Hemostatic compositions
KR101811070B1 (en)Hemostatic sponge
US8475812B2 (en)Gelatin sponge comprising an active ingredient, its preparation and use
US9408945B2 (en)Process for making dry and stable hemostatic compositions
US6454787B1 (en)Collagen hemostatic foam
JP3285887B2 (en) Process for producing a neutralized oxidized cellulose product and its use
KR101735899B1 (en)Biodegradable non-woven material for medical purposes
WO2014106136A1 (en)Lyophilized fibrin sealant for high volume hemorrhage
US12440599B2 (en)Water activated hydrogel-based medical patches, and methods of making and using such patches
US20230355829A1 (en)Water activated hydrogel-based medical patches, and methods of making and using such patches
CN119212741A (en) Water-activated hydrogel-based medical patches, flexible substrates, and methods of making and using such patches
US8741845B1 (en)Lyophilized fibrin sealant for high volume hemorrhage

Legal Events

DateCodeTitleDescription
ASAssignment

Owner name:SUB-Q, INC., CALIFORNIA

Free format text:ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:GREFF, RICHARD J.;REEL/FRAME:013007/0656

Effective date:20020429

ASAssignment

Owner name:BOSTON SCIENTIFIC CORPORATION, MASSACHUSETTS

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PACIFIC VENTURE GROUP II, L.P., CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PVG ASSOCIATES II, L.P., CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PEQUOT PRIVATE EQUITY FUND II, L.P., CONNECTICUT

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:KINGSBURY CAPITAL PARTNERS, L.P. III, CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:KINGSBURY CAPITAL PARTNERS, L.P. IV, CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:HARTZLER, GEOFFREY O., KANSAS

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:WALLACE, GEORGE, CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:CRAGG, ANDREW H., MINNESOTA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:ALLEN FAMILY TRUST DATED 10/12/81, CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:FEUCHTER, BRUCE, CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:BOSTON SCIENTIFIC CORPORATION,MASSACHUSETTS

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PACIFIC VENTURE GROUP II, L.P.,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PVG ASSOCIATES II, L.P.,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:PEQUOT PRIVATE EQUITY FUND II, L.P.,CONNECTICUT

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:KINGSBURY CAPITAL PARTNERS, L.P. III,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:KINGSBURY CAPITAL PARTNERS, L.P. IV,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:HARTZLER, GEOFFREY O.,KANSAS

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:WALLACE, GEORGE,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:CRAGG, ANDREW H.,MINNESOTA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:ALLEN FAMILY TRUST DATED 10/12/81,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

Owner name:FEUCHTER, BRUCE,CALIFORNIA

Free format text:NOTE AND WARRANT PURCHASE AGREEMENT;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:015156/0484

Effective date:20040831

ASAssignment

Owner name:BOSTON SCIENTIFIC SCIMED, INC.,MINNESOTA

Free format text:ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:018420/0029

Effective date:20050504

Owner name:BOSTON SCIENTIFIC SCIMED, INC., MINNESOTA

Free format text:ASSIGNMENT OF ASSIGNORS INTEREST;ASSIGNOR:SUB-Q, INC.;REEL/FRAME:018420/0029

Effective date:20050504

FEPPFee payment procedure

Free format text:PAYOR NUMBER ASSIGNED (ORIGINAL EVENT CODE: ASPN); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

Free format text:PAYER NUMBER DE-ASSIGNED (ORIGINAL EVENT CODE: RMPN); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

STCFInformation on status: patent grant

Free format text:PATENTED CASE

FEPPFee payment procedure

Free format text:PAT HOLDER NO LONGER CLAIMS SMALL ENTITY STATUS, ENTITY STATUS SET TO UNDISCOUNTED (ORIGINAL EVENT CODE: STOL); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

FPAYFee payment

Year of fee payment:4

FEPPFee payment procedure

Free format text:MAINTENANCE FEE REMINDER MAILED (ORIGINAL EVENT CODE: REM.); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

LAPSLapse for failure to pay maintenance fees

Free format text:PATENT EXPIRED FOR FAILURE TO PAY MAINTENANCE FEES (ORIGINAL EVENT CODE: EXP.); ENTITY STATUS OF PATENT OWNER: LARGE ENTITY

STCHInformation on status: patent discontinuation

Free format text:PATENT EXPIRED DUE TO NONPAYMENT OF MAINTENANCE FEES UNDER 37 CFR 1.362

FPLapsed due to failure to pay maintenance fee

Effective date:20200529
[8]ページ先頭
©2009-2025 Movatter.jp